Anti-serum albumin binding variants

ABSTRACT

The invention relates to improved variants of the anti-serum albumin immunoglobulin single variable domain DOM7h-11, as well as ligands and drug conjugates comprising such variants, compositions, nucleic acids, vectors and hosts.

The invention relates to improved variants of the anti-serum albumin immunoglobulin single variable domain DOM7h-11, as well as ligands and drug conjugates comprising such variants, compositions, nucleic acids, vectors and hosts.

BACKGROUND OF THE INVENTION

WO04003019 and WO2008/096158 disclose anti-serum albumin (SA) binding moieties, such as anti-SA immunoglobulin single variable domains (dAbs), which have therapeutically-useful half-lives. These documents disclose monomer anti-SA dAbs as well as multi-specific ligands comprising such dAbs, eg, ligands comprising an anti-SA dAb and a dAb that specifically binds a target antigen, such as TNFR1. Binding moieties are disclosed that specifically bind serum albumins from more than one species, eg human/mouse cross-reactive anti-SA dAbs.

WO05118642 and WO2006/059106 disclose the concept of conjugating or associating an anti-SA binding moiety, such as an anti-SA immunoglobulin single variable domain, to a drug, in order to increase the half-life of the drug. Protein, peptide and NCE (new chemical entity) drugs are disclosed and exemplified. WO2006/059106 discloses the use of this concept to increase the half-life of insulintropic agents, eg, incretin hormones such as glucagon-like peptide (GLP)-1.

Reference is also made to Holt et al, “Anti-Serum albumin domain antibodies for extending the half-lives of short lived drugs”, Protein Engineering, Design & Selection, vol 21, no 5, pp 283-288, 2008.

WO2008/096158 discloses DOM7h-11, which is a good anti-SA dAb. It would be desirable to provide improved dAbs that are variants of DOM7h-11 and that specifically bind serum albumin, preferably albumins from human and non-human species, which would provide utility in animal models of disease as well as for human therapy and/or diagnosis. It would also be desirable to provide for the choice between relatively modest- and high-affinity anti-SA binding moieties (dAbs). Such moieties could be linked to drugs, the anti-SA binding moiety being chosen according to the contemplated end-application. This would allow the drug to be better tailored to treating and/or preventing chronic or acute indications, depending upon the choice of anti-SA binding moiety. It would also be desirable to provide anti-dAbs, that are monomeric or substantially so in solution. This would especially be advantageous when the anti-SA dAb is linked to a binding moiety, eg, a dAb, that specifically binds a cell-surface receptor, such as TNFR1, with the aim of antagonizing the receptor. The monomeric state of the anti-SA dAb is useful in reducing the chance of receptor cross-linking, since multimers are less likely to form which could bind and cross-link receptors (eg, TNFR1) on the cell surface, thus increasing the likelihood of receptor agonism and detrimental receptor signaling.

SUMMARY OF THE INVENTION

Aspects of the present invention solve these problems.

To this end, the present inventors surprisingly found that beneficial mutations can be targeted to the FW2/CDR2 junction (positions 49 to 51, numbering according to Kabat) of DOM7h-11.

In one aspect the invention, therefore, provides an anti-serum albumin (SA) immunoglobulin single variable domain variant of DOM7h-11, wherein the variant comprises at least one mutation in the FW2/CDR2 junction (positions 49 to 51, numbering according to Kabat) compared to DOM7h-11, and wherein the variant has from 2 to 8 changes compared to the amino acid sequence of DOM7h-11.

In one aspect the invention provides an anti-serum albumin (SA) immunoglobulin single variable domain variant of DOM7h-11, wherein the variant comprises a Met at position 32 (numbering according to Kabat) compared to DOM7h-11, and wherein the variant has from 0 to 4 further changes compared to the amino acid sequence of DOM7h-11.

Embodiments of either aspect of the invention provide DOM7h-11 variants of good anti-serum albumin affinities. The choice of variant can allow for tailoring of half-life according to the desired therapeutic and/or prophylactic setting. For example, in one embodiment, the affinity of the variant for serum albumin is relatively high, such that the variant would be useful for inclusion in products that find utility in treating and/or preventing chronic or persistent diseases, conditions, toxicity or other chronic indications. In one embodiment, the affinity of the variant for serum albumin is relatively modest, such that the variant would be useful for inclusion in products that find utility in treating and/or preventing acute diseases, conditions, toxicity or other acute indications. In one embodiment, the affinity of the variant for serum albumin is intermediate, such that the variant would be useful for inclusion in products that find utility in treating and/or preventing acute or chronic diseases, conditions, toxicity or other acute or chronic indications.

It is conceivable that a molecule with an appropriately high affinity and specificity for serum albumin would stay in circulation long enough to have the desired therapeutic effect (Tomlinson, Nature Biotechnology 22, 521-522 (2004)). Here, a high affinity anti-SA variant would stay in serum circulation matching that of the species' serum albumin (WO2008096158). Once in circulation, any fused therapeutic agent to the ALBUDAB™ variant (an ALBUDAB™ is an anti-serum albumin dAb or immunoglobulin single variable domain), be it NCE, peptide or protein, consequently would be able to act longer on its target and exhibit a longer lasting therapeutic effect. This would allow for targeting chronic or persistent diseases without the need of frequent dosing.

A variant with moderate affinity (but specificity to SA) would only stay in serum circulation for a short time (eg, for a few hours or a few days) allowing for the specific targeting of therapeutic targets involved in acute diseases by the fused therapeutic agent.

This way it is possible to tailor the anti-SA-containing product to the therapeutic disease area by choosing an anti-SA variant with the appropriate albumin binding affinity and/or serum half-life.

An aspect of the invention provides a multispecific ligand comprising any anti-SA variant as described above and a binding moiety that specifically binds a target antigen other than SA.

An aspect of the invention provides a fusion product, eg, a fusion protein or fusion with a peptide or NCE (new chemical entity) drug, comprising a polypeptide, protein, peptide or NCE drug fused or conjugated (for an NCE) to any variant as described above, wherein the variant is DOM7h-11-15 or DOM7h-11-15^(S12P) (or a variant having an amino acid that is at least 95, 96, 97, 98 or 99% identical to the amino acid sequence of DOM7h-11-15) or DOM7h-11-12 (or a variant having an amino acid that is at least 95, 96, 97, 98 or 99% identical to the amino acid sequence of DOM7h-11-12). DOM7h-11-15 and DOM7h-11-12 give only a modest drop in affinity when fused or conjugated to partner making them useful in fusion products. DOM7h-11-15^(S12P) is identical to DOM7h-11-15, with the exception that position 12 (numbering according to Kabat) is a proline instead of a serine. This provides advantages set out in WO08052933, including to reduce binding to Protein-L of fusion proteins containing this domain antibody and to facilitate purification. The entire disclosure of WO08052933 is incorporated herein by reference. Similarly, the invention provides a DOM7h-11 variant as disclosed herein wherein the variant comprises an amino acid sequence as set out below with the exception that position 12 (numbering according to Kabat) is a proline. The invention also provides fusion proteins, conjugates or composition comprising such DOM7h-11 variants.

One aspect of the invention provides a variant of DOM7h-11 that comprises an amino acid sequence that is identical to the amino acid sequence of DOM7h-11-15^(S12P) or has up to 4 changes compared to the amino acid sequence of DOM7h-11-15^(S12P), provided that the amino acid sequence of the variant has at least one mutation in the FW2/CDR2 junction (positions 49 to 51, numbering according to Kabat).

An aspect of the invention provides a composition comprising a variant, fusion protein or ligand of any preceding aspect and a pharmaceutically acceptable diluent, carrier, excipient or vehicle.

An aspect of the invention provides a method of treating or preventing a disease or disorder in a patient, comprising administering at least one dose of a variant according to any aspect or embodiment of the invention to said patient.

An aspect of the invention provides a polypeptide fusion or conjugate comprising an anti-serum albumin dAb as disclosed herein (eg, DOM7h-11-15 or DOM7h-11-3 or DOM7h-11-15^(S12P) or DOM7h-11-15^(S12P) with up to 4 changes compared to the amino acid sequence of DOM7h-11-15^(S12P)) and an incretin or insulinotropic agent, eg, exendin-4, GLP-1(7-37), GLP-1(6-36) or any incretin or insulinotropic agent disclosed in WO06/059106, these agents being explicitly incorporated herein by reference as though written herein for inclusion in the present invention and claims below.

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1: Amino-acid sequence alignment for DOM7h-11 (SEQ ID NO: 421) variant dAbs. A “.” at a particular position indicates the same amino as found in DOM7h-11 at that position. The CDRs are indicated by underlining and bold text (the first underlined sequence is CDR1, the second underlined sequence is CDR2 and the third underlined sequence is CDR3). The figure comprises the following variants: DOM 7h-11-12 (SEQ ID NO:1), DOM 7h-11-15 (SEQ ID NO:2), DOM 7h-11-18 (SEQ ID NO:3), DOM 7h-11-19 (SEQ ID NO:4), and DOM 7h-11-3 (SEQ ID NO: 5).

FIG. 2: Kinetic parameters of DOM7h-11 variants. KD units=nM; Kd units=sec⁻¹; Ka units=M⁻¹ sec⁻¹. The notation A e-B means A×10^(−B) and C e D means C×10^(D). The overall kinetic ranges in various species, as supported by the examples below, are indicated. Optional ranges are also provided for use in particular therapeutic settings (acute or chronic indications, conditions or diseases and “intermediate” for use in both chronic and acute settings). High affinity dAbs and products comprising these are useful for chronic settings. Medium affinity dAbs and products comprising these are useful for intermediate settings. Low affinity dAbs and products comprising these are useful for acute settings. The affinity in this respect is the affinity for serum albumin. Various example anti-serum dAbs and fusion proteins are listed, and these support the ranges disclosed. Many of the examples have favourable kinetics in human and one or more non-human animals (eg, in human and Cynomolgus monkey and/or mouse). Choice of dAb or product comprising this can be tailored, according to the invention, depending on the setting (eg, chronic or acute) to be treated therapeutically.

DETAILED DESCRIPTION OF THE INVENTION

Within this specification the invention has been described, with reference to embodiments, in a way which enables a clear and concise specification to be written. It is intended and should be appreciated that embodiments may be variously combined or separated without parting from the invention.

Unless defined otherwise, all technical and scientific terms used herein have the same meaning as commonly understood by one of ordinary skill in the art (e.g., in cell culture, molecular genetics, nucleic acid chemistry, hybridization techniques and biochemistry). Standard techniques are used for molecular, genetic and biochemical methods (see generally, Sambrook et al., Molecular Cloning: A Laboratory Manual, 2d ed. (1989) Cold Spring Harbor Laboratory Press, Cold Spring Harbor, N.Y. and Ausubel et al., Short Protocols in Molecular Biology (1999) 4^(th) Ed, John Wiley & Sons, Inc. which are incorporated herein by reference) and chemical methods.

As used herein, the term “antagonist of Tumor Necrosis Factor Receptor 1 (TNFR1)” or “anti-TNFR1 antagonist” or the like refers to an agent (e.g., a molecule, a compound) which binds TNFR1 and can inhibit a (i.e., one or more) function of TNFR1. For example, an antagonist of TNFR1 can inhibit the binding of TNFα to TNFR1 and/or inhibit signal transduction mediated through TNFR1. Accordingly, TNFR1-mediated processes and cellular responses (e.g., TNFα-induced cell death in a standard L929 cytotoxicity assay) can be inhibited with an antagonist of TNFR1.

A “patient” is any animal, eg, a mammal, eg, a non-human primate (such as a baboon, rhesus monkey or Cynomolgus monkey), mouse, human, rabbit, rat, dog, cat or pig. In one embodiment, the patient is a human.

As used herein, “peptide” refers to about two to about 50 amino acids that are joined together via peptide bonds.

As used herein, “polypeptide” refers to at least about 50 amino acids that are joined together by peptide bonds. Polypeptides generally comprise tertiary structure and fold into functional domains.

As used herein an antibody refers to IgG, IgM, IgA, IgD or IgE or a fragment (such as a Fab, F(ab′)₂, Fv, disulphide linked Fv, scFv, closed conformation multispecific antibody, disulphide-linked scFv, diabody) whether derived from any species naturally producing an antibody, or created by recombinant DNA technology; whether isolated from serum, B-cells, hybridomas, transfectomas, yeast or bacteria.

As used herein, “antibody format” refers to any suitable polypeptide structure in which one or more antibody variable domains can be incorporated so as to confer binding specificity for antigen on the structure. A variety of suitable antibody formats are known in the art, such as, chimeric antibodies, humanized antibodies, human antibodies, single chain antibodies, bispecific antibodies, antibody heavy chains, antibody light chains, homodimers and heterodimers of antibody heavy chains and/or light chains, antigen-binding fragments of any of the foregoing (e.g., a Fv fragment (e.g., single chain Fv (scFv), a disulfide bonded Fv), a Fab fragment, a Fab′ fragment, a F(ab′)2 fragment), a single antibody variable domain (e.g., a dAb, V_(H), V_(HH), V_(L)), and modified versions of any of the foregoing (e.g., modified by the covalent attachment of polyethylene glycol or other suitable polymer or a humanized V_(HH)).

The phrase “immunoglobulin single variable domain” refers to an antibody variable domain (V_(H), V_(HH), V_(L)) that specifically binds an antigen or epitope independently of different V regions or domains. An immunoglobulin single variable domain can be present in a format (e.g., homo- or hetero-multimer) with other variable regions or variable domains where the other regions or domains are not required for antigen binding by the single immunoglobulin variable domain (i.e., where the immunoglobulin single variable domain binds antigen independently of the additional variable domains). A “domain antibody” or “dAb” is the same as an “immunoglobulin single variable domain” as the term is used herein. A “single immunoglobulin variable domain” is the same as an “immunoglobulin single variable domain” as the term is used herein. A “single antibody variable domain” or an “antibody single variable domain” is the same as an “immunoglobulin single variable domain” as the term is used herein. An immunoglobulin single variable domain is in one embodiment a human antibody variable domain, but also includes single antibody variable domains from other species such as rodent (for example, as disclosed in WO 00/29004, the contents of which are incorporated herein by reference in their entirety), nurse shark and Camelid V_(HH) dAbs. Camelid V_(HH) are immunoglobulin single variable domain polypeptides that are derived from species including camel, llama, alpaca, dromedary, and guanaco, which produce heavy chain antibodies naturally devoid of light chains. The V_(HH) may be humanized.

A “domain” is a folded protein structure which has tertiary structure independent of the rest of the protein. Generally, domains are responsible for discrete functional properties of proteins, and in many cases may be added, removed or transferred to other proteins without loss of function of the remainder of the protein and/or of the domain. A “single antibody variable domain” is a folded polypeptide domain comprising sequences characteristic of antibody variable domains. It therefore includes complete antibody variable domains and modified variable domains, for example, in which one or more loops have been replaced by sequences which are not characteristic of antibody variable domains, or antibody variable domains which have been truncated or comprise N- or C-terminal extensions, as well as folded fragments of variable domains which retain at least the binding activity and specificity of the full-length domain.

In the instant application, the term “prevention” and “preventing” involves administration of the protective composition prior to the induction of the disease or condition. “Treatment” and “treating” involves administration of the protective composition after disease or condition symptoms become manifest. “Suppression” or “suppressing” refers to administration of the composition after an inductive event, but prior to the clinical appearance of the disease or condition.

As used herein, the term “dose” refers to the quantity of ligand administered to a subject all at one time (unit dose), or in two or more administrations over a defined time interval. For example, dose can refer to the quantity of ligand (e.g., ligand comprising an immunoglobulin single variable domain that binds target antigen) administered to a subject over the course of one day (24 hours) (daily dose), two days, one week, two weeks, three weeks or one or more months (e.g., by a single administration, or by two or more administrations). The interval between doses can be any desired amount of time. The term “pharmaceutically effective” when referring to a dose means sufficient amount of the ligand, domain or pharmaceutically active agent to provide the desired effect. The amount that is “effective” will vary from subject to subject, depending on the age and general condition of the individual, the particular drug or pharmaceutically active agent and the like. Thus, it is not always possible to specify an exact “effective” amount applicable for all patients. However, an appropriate “effective” dose in any individual case may be determined by one of ordinary skill in the art using routine experimentation.

Methods for pharmacokinetic analysis and determination of ligand (eg, single variable domain, fusion protein or multi-specific ligand) half-life will be familiar to those skilled in the art. Details may be found in Kenneth, A et al: Chemical Stability of Pharmaceuticals: A Handbook for Pharmacists and in Peters et al, Pharmacokinetc analysis: A Practical Approach (1996). Reference is also made to “Pharmacokinetics”, M Gibaldi & D Perron, published by Marcel Dekker, 2nd Rev. ex edition (1982), which describes pharmacokinetic parameters such as t alpha and t beta half lives and area under the curve (AUC). Optionally, all pharmacokinetic parameters and values quoted herein are to be read as being values in a human. Optionally, all pharmacokinetic parameters and values quoted herein are to be read as being values in a mouse or rat or Cynomolgus monkey.

Half lives (t½ alpha and t½ beta) and AUC can be determined from a curve of serum concentration of ligand against time. The WinNonlin analysis package, eg version 5.1 (available from Pharsight Corp., Mountain View, Calif. 94040, USA) can be used, for example, to model the curve. When two-compartment modeling is used, in a first phase (the alpha phase) the ligand is undergoing mainly distribution in the patient, with some elimination. A second phase (beta phase) is the phase when the ligand has been distributed and the serum concentration is decreasing as the ligand is cleared from the patient. The t alpha half life is the half life of the first phase and the t beta half life is the half life of the second phase. Thus, in one embodiment, in the context of the present invention, the variable domain, fusion protein or ligand has a tα half-life in the range of (or of about) 15 minutes or more. In one embodiment, the lower end of the range is (or is about) 30 minutes, 45 minutes, 1 hour, 2 hours, 3 hours, 4 hours, 5 hours, 6 hours, 7 hours, 10 hours, 11 hours or 12 hours. In addition, or alternatively, the variable domain, fusion protein or ligand according to the invention will have a tα half life in the range of up to and including 12 hours (or about 12 hours). In one embodiment, the upper end of the range is (or is about) 11, 10, 9, 8, 7, 6 or 5 hours. An example of a suitable range is (or is about) 1 to 6 hours, 2 to 5 hours or 3 to 4 hours.

In one embodiment, the present invention provides the variable domain, fusion protein or ligand according to the invention has a tβ half-life in the range of (or of about) 2.5 hours or more. In one embodiment, the lower end of the range is (or is about) 3 hours, 4 hours, 5 hours, 6 hours, 7 hours, 10 hours, 11 hours, or 12 hours. In addition, or alternatively, the tβ half-life is (or is about) up to and including 21 or 25 days. In one embodiment, the upper end of the range is (or is about) 12 hours, 24 hours, 2 days, 3 days, 5 days, 10 days, 15 days, 19 days, 20 days, 21 days or 22 days. For example, the variable domain, fusion protein or ligand according to the invention will have a tβ half life in the range 12 to 60 hours (or about 12 to 60 hours). In a further embodiment, it will be in the range 12 to 48 hours (or about 12 to 48 hours). In a further embodiment still, it will be in the range 12 to 26 hours (or about 12 to 26 hours).

As an alternative to using two-compartment modeling, the skilled person will be familiar with the use of non-compartmental modeling, which can be used to determine terminal half-lives (in this respect, the term “terminal half-life” as used herein means a terminal half-life determined using non-compartmental modeling). The WinNonlin analysis package, eg version 5.1 (available from Pharsight Corp., Mountain View, Calif. 94040, USA) can be used, for example, to model the curve in this way. In this instance, in one embodiment the single variable domain, fusion protein or ligand has a terminal half life of at least (or at least about) 8 hours, 10 hours, 12 hours, 15 hours, 28 hours, 20 hours, 1 day, 2 days, 3 days, 7 days, 14 days, 15 days, 16 days, 17 days, 18 days, 19 days, 20 days, 21 days, 22 days, 23 days, 24 days or 25 days. In one embodiment, the upper end of this range is (or is about) 24 hours, 48 hours, 60 hours or 72 hours or 120 hours. For example, the terminal half-life is (or is about) from 8 hours to 60 hours, or 8 hours to 48 hours or 12 to 120 hours, eg, in man.

In addition, or alternatively to the above criteria, the variable domain, fusion protein or ligand according to the invention has an AUC value (area under the curve) in the range of (or of about) 1 mg·min/ml or more. In one embodiment, the lower end of the range is (or is about) 5, 10, 15, 20, 30, 100, 200 or 300 mg·min/ml. In addition, or alternatively, the variable domain, fusion protein or ligand according to the invention has an AUC in the range of (or of about) up to 600 mg·min/ml. In one embodiment, the upper end of the range is (or is about) 500, 400, 300, 200, 150, 100, 75 or 50 mg·min/ml. Advantageously the variable domain, fusion protein or ligand will have an AUC in (or about in) the range selected from the group consisting of the following: 15 to 150 mg·min/ml, 15 to 100 mg·min/ml, 15 to 75 mg·min/ml, and 15 to 50 mg·min/ml.

“Surface Plasmon Resonance”: Competition assays can be used to determine if a specific antigen or epitope, such as human serum albumin, competes with another antigen or epitope, such as cynomolgus serum albumin, for binding to a serum albumin binding ligand described herein, such as a specific dAb. Similarly competition assays can be used to determine if a first ligand such as dAb, competes with a second ligand such as a dAb for binding to a target antigen or epitope. The term “competes” as used herein refers to substance, such as a molecule, compound, preferably a protein, which is able to interfere to any extent with the specific binding interaction between two or more molecules. The phrase “does not competitively inhibit” means that substance, such as a molecule, compound, preferably a protein, does not interfere to any measurable or significant extent with the specific binding interaction between two or more molecules. The specific binding interaction between two or more molecules preferably includes the specific binding interaction between a single variable domain and its cognate partner or target. The interfering or competing molecule can be another single variable domain or it can be a molecule that is structurally and/or functionally similar to a cognate partner or target.

The term “binding moiety” refers to a domain that specifically binds an antigen or epitope independently of a different epitope or antigen binding domain. A binding moiety may be a domain antibody (dAb) or may be a domain which is a derivative of a non-immunoglobulin protein scaffold, eg, a scaffold selected from the group consisting of CTLA-4, lipocalin, SpA, an adnectin, affibody, an avimer, GroEl, transferrin, GroES and fibronectin, which binds to a ligand other than the natural ligand (in the case of the present invention, the moiety binds serum albumin). See WO2008/096158, which discloses examples of protein scaffolds and methods for selecting antigen or epitope-specific binding domains from repertoires (see Examples 17 to 25). These specific disclosures of WO2008/096158 are expressly incorporated herein by reference as though explicitly written herein and for use with the present invention, and it is contemplated that any part of such disclosure can be incorporated into one or more claims herein).

In one aspect, the invention provides an anti-serum albumin (SA) immunoglobulin single variable domain variant of DOM7h-11, wherein the variant comprises at least one mutation in the FW2/CDR2 junction (positions 49 to 51, numbering according to Kabat) compared to DOM7h-11, and wherein the variant has from 2 to 8 changes compared to the amino acid sequence of DOM7h-11. Optionally, position 49 (according to Kabat) is Leu. Additionally or alternatively, position 50 (according to Kabat) is optionally Ala or Trp. Additionally or alternatively, position 51 (according to Kabat) is optionally Phe or Asn. In one embodiment, the variant comprises a mutation at each of positions 49, 50 and 51 (numbering according to Kabat) compared to DOM7h-11. In one embodiment, the variant comprises a LFG motif, where L is at position 49 (numbering according to Kabat), wherein L, F and G are Leu, Phe and Gly respectively.

In one embodiment, the variant comprises an amino acid sequence that is identical to the amino acid sequence of a single variable domain selected from DOM7h-11-3, DOM7h-11-15, DOM7h-11-12 and DOM7h-11-19 or has up to 4 changes compared to the selected amino acid sequence, provided that the amino acid sequence of the variant has at least one mutation in the FW2/CDR2 junction as defined above. In one embodiment, the variant comprises an amino acid sequence that is identical to the amino acid sequence of DOM7h-11-15^(S12P) or has up to 4 changes compared to the amino acid sequence of DOM7h-11-15^(S12P), provided that the amino acid sequence of the variant has at least one mutation in the FW2/CDR2 junction (positions 49 to 51, numbering according to Kabat). In one embodiment, the variant comprises an amino acid sequence that is identical to the amino acid sequence of a single variable domain selected from DOM7h-11-3, or has up to 4 changes compared to the selected amino acid sequence, provided that the amino acid sequence of the variant has L at position 49, W at position 50 and N at position 51. In one embodiment, the variant comprises an amino acid sequence that is identical to the amino acid sequence of a single variable domain selected from DOM7h-11-12, or has up to 4 changes compared to the selected amino acid sequence, provided that the amino acid sequence of the variant has M at position 32 and L at position 49. In one embodiment, the variant comprises an amino acid sequence that is identical to the amino acid sequence of a single variable domain selected from DOM7h-11-15 or DOM7h-11-15^(S12P), or has up to 4 changes compared to the selected amino acid sequence, provided that the amino acid sequence of the variant has M at position 32, L at position 49, A at position 50 and F at position 51. In one embodiment, the variant comprises an amino acid sequence that is identical to the amino acid sequence of a single variable domain selected from DOM7h-11-18, or has up to 4 changes compared to the selected amino acid sequence, provided that the amino acid sequence of the variant has M at position 32 and H at position 87. In one embodiment, the variant comprises an amino acid sequence that is identical to the amino acid sequence of a single variable domain selected from DOM7h-11-19, or has up to 4 changes compared to the selected amino acid sequence, provided that the amino acid sequence of the variant has M at position 32, L at position 49 and T at position 91. All numbering in this paragraph is according to Kabat.

An aspect of the invention provides an anti-serum albumin (SA) immunoglobulin single variable domain variant of DOM7h-11, wherein the variant comprises a Met at position 32 (numbering according to Kabat) compared to DOM7h-11, and wherein the variant has from 0 to 4 further changes compared to the amino acid sequence of DOM7h-11. Optionally, the variant comprises at least one mutation in the FW2/CDR2 junction (positions 49 to 51, numbering according to Kabat) compared to DOM7h-11.

In one embodiment of any aspect of the invention, the variant comprises at least one mutation compared to DOM7h-11 selected from the following

Position 49=L, Position 50=A or W, Position 51=F or N, Position 87=H, and Position 91=T.

In one embodiment, the variant comprises an amino acid sequence that is identical to the amino acid sequence of a single variable domain selected from DOM7h-11-12, DOM7h-11-15, DOM7h-11-15^(S12P), DOM7h-11-18 and DOM7h-11-19 or has up to 4 changes compared to the selected amino acid sequence, provided that the amino acid sequence of the variant has Met at position 32.

In one embodiment, the variant comprises one or more of the following kinetic characteristics:—

-   -   (a) The variant comprises a binding site that specifically binds         human SA with a dissociation constant (KD) from (or from about)         0.1 to (or to about) 10000 nM, optionally from (or from about) 1         to (or to about) 6000 nM, as determined by surface plasmon         resonance;     -   (b) The variant comprises a binding site that specifically binds         human SA with an off-rate constant (K_(d)) from (or from about)         1.5×10⁻⁴ to (or to about) 0.1 sec⁻¹, optionally from (or from         about) 3×10⁻⁴ to (or to about) 0.1 sec⁻¹ as determined by         surface plasmon resonance;     -   (c) The variant comprises a binding site that specifically binds         human SA with an on-rate constant (K_(a)) from (or from about)         2×10⁶ to (or to about) 1×10⁴M⁻¹ sec⁻¹, optionally from (or from         about) 1×10⁶ to (or to about) 2×10⁴M⁻¹ sec⁻¹ as determined by         surface plasmon resonance;     -   (d) The variant comprises a binding site that specifically binds         Cynomolgus monkey SA with a dissociation constant (KD) from (or         from about) 0.1 to (or to about) 10000 nM, optionally from (or         from about) 1 to (or to about) 6000 nM, as determined by surface         plasmon resonance;     -   (e) The variant of any preceding claim, wherein the variant         comprises a binding site that specifically binds Cynomolgus         monkey SA with an off-rate constant (K_(d)) from (or from about)         1.5×10⁻⁴ to (or to about) 0.1 sec⁻¹, optionally from (or from         about) 3×10⁻⁴ to (or to about) 0.1 sec⁻¹ as determined by         surface plasmon resonance;     -   (f) The variant of any preceding claim, wherein the variant         comprises a binding site that specifically binds Cynomolgus         monkey SA with an on-rate constant (K_(a)) from (or from about)         2×10⁶ to (or to about) 1×10⁴M⁻¹ sec⁻¹, optionally from (or from         about) 1×10⁶ to (or to about) 5×10³M⁻¹ sec⁻¹ as determined by         surface plasmon resonance;     -   (g) The variant comprises a binding site that specifically binds         rat SA with a dissociation constant (KD) from (or from about) 1         to (or to about) 10000 nM, optionally from (or from about) 20 to         (or to about) 6000 nM, as determined by surface plasmon         resonance;     -   (h) The variant comprises a binding site that specifically binds         rat SA with an off-rate constant (K_(d)) from (or from about)         2×10⁻³ to (or to about) 0.15 sec⁻¹, optionally from (or from         about) 9×10⁻³ to (or to about) 0.14 sec⁻¹ as determined by         surface plasmon resonance;     -   (i) The variant comprises a binding site that specifically binds         rat SA with an on-rate constant (K_(a)) from (or from about)         2×10⁶ to (or to about) 1×10⁴ M⁻¹ sec⁻¹, optionally from (or from         about) 1×10⁶ to (or to about) 3×10⁴ M⁻¹ sec⁻¹ as determined by         surface plasmon resonance;     -   (j) The variant comprises a binding site that specifically binds         mouse SA with a dissociation constant (KD) from (or from about)         1 to (or to about) 10000 nM as determined by surface plasmon         resonance;     -   (k) The variant comprises a binding site that specifically binds         mouse SA with an off-rate constant (K_(d)) from (or from about)         2×10⁻³ to (or to about) 0.15 sec⁻¹ as determined by surface         plasmon resonance; and/or     -   (l) The variant comprises a binding site that specifically binds         mouse SA with an on-rate constant (K_(a)) from (or from about)         2×10⁶ to (or to about) 1×10⁴ M⁻¹ sec⁻¹, optionally from (or from         about) 2×10⁶ to (or to about) 1.5×10⁴ M⁻¹ sec⁻¹ as determined by         surface plasmon resonance.     -   Optionally, the variant has     -   I: a KD according to (a) and (d), a K_(d) according to (b) and         (e), and a K_(a) according to (c) and (f); or     -   II: a KD according to (a) and (g), a K_(d) according to (b) and         (h), and a K_(a) according to (c) and (i); or     -   III: a KD according to (a) and (j), a K_(d) according to (b) and         (k), and a K_(a) according to (c) and (1); or     -   IV: kinetics according to I and II; or     -   V: kinetics according to I and III; or     -   VI: kinetics according to I, II and III.

The invention also provides a ligand comprising a variant of any preceding aspect or embodiment of the invention. For example, the ligand can be a dual-specific ligand (see WO04003019 for examples of dual-specific ligands). In one aspect, the invention provides a multispecific ligand comprising an anti-SA variant of any preceding aspect or embodiment of the invention and a binding moiety that specifically binds a target antigen other than SA. The binding moiety can be any binding moiety that specifically binds a target, eg, the moiety is an antibody, antibody fragment, scFv, Fab, dAb or a binding moiety comprising a non-immunoglobulin protein scaffold. Such moieties are disclosed in detail in WO2008/096158 (see examples 17 to 25, which disclosure is incorporated herein by reference). Examples of non-immunoglobulin scaffolds are CTLA-4, lipocallin, staphylococcal protein A (spA), Affibody™ Avimers™, adnectins, GroEL and fibronectin.

In one embodiment, a linker is provided between the anti-target binding moiety and the anti-SA single variant, the linker comprising the amino acid sequence AST, optionally ASTSGPS. Alternative linkers are described in WO2007085814 (incorporated herein by reference) and WO2008/096158 (see the passage at page 135, line 12 to page 140, line 14, which disclosure and all sequences of linkers are expressly incorporated herein by reference as though explicitly written herein and for use with the present invention, and it is contemplated that any part of such disclosure can be incorporated into one or more claims herein).

In one embodiment of the multispecific ligand, the target antigen may be, or be part of, polypeptides, proteins or nucleic acids, which may be naturally occurring or synthetic. In this respect, the ligand of the invention may bind the target antigen and act as an antagonist or agonist (e.g., EPO receptor agonist). One skilled in the art will appreciate that the choice is large and varied. They may be for instance, human or animal proteins, cytokines, cytokine receptors, where cytokine receptors include receptors for cytokines, enzymes, co-factors for enzymes or DNA binding proteins. Suitable cytokines and growth factors include, but are preferably not limited to: ApoE, Apo-SAA, BDNF, Cardiotrophin-1, EGF, EGF receptor, ENA-78, Eotaxin, Eotaxin-2, Exodus-2, EpoR, FGF-acidic, FGF-basic, fibroblast growth factor-10, FLT3 ligand, Fractalkine (CX3C), GDNF, G-CSF, GM-CSF, GF-β1, insulin, IFN-γ, IGF-I, IGF-II, IL-1α, IL-113, IL-2, IL-3, IL-4, IL-5, IL-6, IL-7, IL-8 (72 a.a.), IL-8 (77 a.a.), IL-9, IL-10, IL-11, IL-12, IL-13, IL-15, IL-16, IL-17, IL-18 (IGIF), Inhibin α, Inhibin β, IP-10, keratinocyte growth factor-2 (KGF-2), KGF, Leptin, LIF, Lymphotactin, Mullerian inhibitory substance, monocyte colony inhibitory factor, monocyte attractant protein, M-CSF, MDC (67 a.a.), MDC (69 a.a.), MCP-1 (MCAF), MCP-2, MCP-3, MCP-4, MDC (67 a.a.), MDC (69 a.a.), MIG, MIP-1α, MIP-1β, MIP-3α, MIP-3β, MIP-4, myeloid progenitor inhibitor factor-1 (MPIF-1), NAP-2, Neurturin, Nerve growth factor, β-NGF, NT-3, NT-4, Oncostatin M, PDGF-AA, PDGF-AB, PDGF-BB, PF-4, RANTES, SDF1α, SDF1β, SCF, SCGF, stem cell factor (SCF), TARC, TGF-α, TGF-β, TGF-β2, TGF-β3, tumour necrosis factor (TNF), TNF-α, TNF-β, TNF receptor I, TNF receptor II, TNIL-1, TPO, VEGF, VEGF receptor 1, VEGF receptor 2, VEGF receptor 3, GCP-2, GRO/MGSA, GRO-β, GRO-γ, HCC1, 1-309, HER 1, HER 2, HER 3 and HER 4, CD4, human chemokine receptors CXCR4 or CCR5, non-structural protein type 3 (NS3) from the hepatitis C virus, TNF-alpha, IgE, IFN-gamma, MMP-12, CEA, H. pylori, TB, influenza, Hepatitis E, MMP-12, internalizing receptors that are over-expressed on certain cells, such as the epidermal growth factor receptor (EGFR), ErBb2 receptor on tumor cells, an internalising cellular receptor, LDL receptor, FGF2 receptor, ErbB2 receptor, transferrin receptor, PDGF receptor, VEGF receptor, PsmAr, an extracellular matrix protein, elastin, fibronectin, laminin, al-antitrypsin, tissue factor protease inhibitor, PDK1, GSK1, Bad, caspase-9, Forkhead, an antigen of Helicobacter pylori, an antigen of Mycobacterium tuberculosis, and an antigen of influenza virus. It will be appreciated that this list is by no means exhaustive.

In one embodiment, the multispecific ligand comprises an anti-SA dAb variant of the invention and an anti-TNFR1 binding moiety, eg, an anti-TNFR1 dAb. Optionally, the ligand has only one anti-TNFR1 binding moiety (eg, dAb) to reduce the chance of receptor cross-linking. In one embodiment, the anti-SA dAb variant is DOM7h-11-3 or DOM7h-11-15 or DOM7h-11-15^(S12P).

In one embodiment, the anti-TNFR1 binding moiety is DOM1h-131-206 disclosed in WO2008149148 (the amino acid sequence of which and the nucleotide sequence of which, as disclosed in that PCT application, are expressly incorporated herein by reference as though explicitly written herein and for use with the present invention, and it is contemplated that any part of such disclosure can be incorporated into one or more claims herein). In one embodiment, the multispecific ligand comprises or consists of the amino acid sequence of DOM1h-131-206 and the amino acid sequence of DOM7h-11-3 or DOM7h-11-15 or DOM7h-11-15^(S12P).

In one embodiment, the anti-TNFR1 binding moiety or dAb is any such moiety or dAb disclosed in co-pending application U.S. Ser. No. 61/153,746, the disclosure of which is incorporated herein by reference. In one embodiment, the anti-TNFR1 binding moiety comprises an amino acid sequence that is at least 95% identical to the amino acid sequence of DOM1h-574-156, DOM1h-574-72, DOM1h-574-109, DOM1h-574-138, DOM1h-574-162 or DOM1h-574-180 or the amino acid sequence of any anti-TNFR1 dAb disclosed in Table 3. In one embodiment, the multispecific ligand comprises or consists of the amino acid sequence of DOM1h-574-156 and the amino acid sequence of DOM7h-11-3 or DOM7h-11-15 or DOM7h-11-15^(S12P).

In one embodiment, the ligand of the invention is a fusion protein comprising a variant of the invention fused directly or indirectly to one or more polypeptides. For example, the fusion protein can be a “drug fusion” as disclosed in WO2005/118642 (the disclosure of which is incorporated herein by reference), comprising a variant of the invention and a polypeptide drug as defined in that PCT application.

As used herein, “drug” refers to any compound (e.g., small organic molecule, nucleic acid, polypeptide) that can be administered to an individual to produce a beneficial, therapeutic or diagnostic effect through binding to and/or altering the function of a biological target molecule in the individual. The target molecule can be an endogenous target molecule encoded by the individual's genome (e.g. an enzyme, receptor, growth factor, cytokine encoded by the individual's genome) or an exogenous target molecule encoded by the genome of a pathogen (e. g. an enzyme encoded by the genome of a virus, bacterium, fungus, nematode or other pathogen). Suitable drugs for use in fusion proteins and conjugates comprising an anti-SA dAb variant of the invention are disclosed in WO2005/118642 and WO2006/059106 (the entire disclosures of which are incorporated herein by reference, and including the entire list of specific drugs as though this list were expressly written herein, and it is contemplated that such incorporation provides disclosure of specific drugs for inclusion in claims herein). For example, the drug can be glucagon-like peptide 1 (GLP-1) or a variant, interferon alpha 2b or a variant or exendin-4 or a variant.

In one embodiment, the invention provides a drug conjugate as defined and disclosed in WO2005/118642 and WO2006/059106, wherein the conjugate comprises a variant of the invention. In one example, the drug is covalently linked to the variant (eg, the variant and the drug are expressed as part of a single polypeptide). Alternatively, in an example, the drug is non-covalently bonded or associated with the variant. The drug can be covalently or noncovalently bonded to the variant directly or indirectly (e.g., through a suitable linker and/or noncovalent binding of complementary binding partners (e.g., biotin and avidin)). When complementary binding partners are employed, one of the binding partners can be covalently bonded to the drug directly or through a suitable linker moiety, and the complementary binding partner can be covalently bonded to the variant directly or through a suitable linker moiety. When the drug is a polypeptide or peptide, the drug composition can be a fusion protein, wherein the polypeptide or peptide, drug and the polypeptide binding moiety are discrete parts (moieties) of a continuous polypeptide chain. As described herein, the polypeptide binding moieties and polypeptide drug moieties can be directly bonded to each other through a peptide bond, or linked through a suitable amino acid, or peptide or polypeptide linker.

A ligand which contains one single variable domain (monomer) variant of the invention or more than one single variable domain (multimer, fusion protein, conjugate, and dual specific ligand as defined herein) which specifically binds to serum albumin, can further comprise one or more entities selected from, but preferably not limited to a label, a tag, an additional single variable domain, a dAb, an antibody, an antibody fragment, a marker and a drug. One or more of these entities can be located at either the COOH terminus or at the N terminus or at both the N terminus and the COOH terminus of the ligand comprising the single variable domain, (either immunoglobulin or non-immunoglobulin single variable domain). One or more of these entities can be located at either the COOH terminus, or the N terminus, or both the N terminus and the COOH terminus of the single variable domain which specifically binds serum albumin of the ligand which contains one single variable domain (monomer) or more than one single variable domains (multimer, fusion protein, conjugate, and dual specific ligand as defined herein). Non-limiting examples of tags which can be positioned at one or both of these termini include a HA, his or a myc tag. The entities, including one or more tags, labels and drugs, can be bound to the ligand which contains one single variable domain (monomer) or more than one single variable domain (multimer, fusion protein, conjugate, and dual specific ligand as defined herein), which binds serum albumin, either directly or through linkers as described above.

An aspect of the invention provides a fusion product, eg, a fusion protein or fusion with a peptide or conjugate with an NCE (new chemical entity) drug, comprising a polypeptide drug fused or conjugated (for an NCE) to any variant as described above, optionally wherein the variant is DOM7h-11-15 or DOM7h-11-15^(S12P) (or a variant having an amino acid that is at least 95, 96, 97, 98 or 99% identical to the amino acid sequence of DOM7h-11-15 or DOM7h-11-15^(S12P)) or DOM7h-11-12 (or a variant having an amino acid that is at least 95, 96, 97, 98 or 99% identical to the amino acid sequence of DOM7h-11-15 or DOM7h-11-15^(S12P)). DOM7h-11-15, DOM7h-11-15^(S12P) and DOM7h-11-12 give only a modest drop in affinity when fused or conjugated to partner, making them useful in fusion products.

The invention provides a composition comprising a variant, fusion protein, conjugate or ligand of any aspect of the invention and a pharmaceutically acceptable diluent, carrier, excipient or vehicle.

Also encompassed herein is an isolated nucleic acid encoding any of the variants, fusion proteins, conjugates or ligands described herein, e.g., a ligand which contains one single variable domain (monomer) variant of the invention or more than one single variable domain (e.g., multimer, fusion protein, conjugate, and dual specific ligand as defined herein) variant which specifically binds to serum albumin, or which specifically binds both human serum albumin and at least one non-human serum albumin, or functionally active fragments thereof. Also encompassed herein is a vector and/or an expression vector, a host cell comprising the vector, e.g., a plant or animal cell and/or cell line transformed with a vector, a method of expressing and/or producing one or more variants, fusion proteins or ligands which contains one single variable domain (monomer) variant or more than one single variable domain variants (e.g., multimer, fusion protein, conjugate, and dual specific ligand as defined herein) which specifically binds to serum albumin, or fragment(s) thereof encoded by said vectors, including in some instances culturing the host cell so that the one or more variants, fusion proteins or ligands or fragments thereof are expressed and optionally recovering the ligand which contains one single variable domain (monomer) or more than one single variable domain (e.g., multimer, fusion protein, conjugate, and dual specific ligand as defined herein) which specifically binds to serum albumin, from the host cell culture medium. Also encompassed are methods of contacting a ligand described herein with serum albumin, including serum albumin and/or non-human serum albumin(s), and/or one or more targets other than serum albumin, where the targets include biologically active molecules, and include animal proteins, cytokines as listed above, and include methods where the contacting is in vitro as well as administering any of the variants, fusion proteins or ligands described herein to an individual host animal or cell in vivo and/or ex vivo. Preferably, administering ligands described herein which comprises a single variable domain (immunoglobulin or non-immunoglobulin) directed to serum albumin and/or non-human serum albumin(s), and one or more domains directed to one or more targets other than serum albumin, will increase the half life, including the T beta and/or terminal half life, of the anti-target ligand. Nucleic acid molecules encoding the variants, fusion proteins or single domain containing ligands or fragments thereof, including functional fragments thereof, are contemplated herein. Vectors encoding the nucleic acid molecules, including but preferably not limited to expression vectors, are contemplated herein, as are host cells from a cell line or organism containing one or more of these expression vectors. Also contemplated are methods of producing any variant, fusion protein or ligand, including, but preferably not limited to any of the aforementioned nucleic acids, vectors and host cells.

An aspect of the invention provides a nucleic acid comprising a nucleotide sequence encoding a variant according to the invention or a multispecific ligand of the invention or fusion protein of the invention.

An aspect of the invention provides a nucleic acid comprising the nucleotide sequence of a DOM7h-11 variant selected from DOM7h-11-3, DOM7h-11-15, DOM7h-11-15^(S12P), DOM7h-11-12, DOM7h-11-18 and DOM7h-11-19 or a nucleotide sequence that is at least 70, 75, 80, 85, 90, 95, 96, 97, 98 or 99% identical to said selected sequence.

An aspect of the invention provides a vector comprising the nucleic acid of the invention. An aspect of the invention provides an isolated host cell comprising the vector.

Reference is made to WO2008/096158 for details of library vector systems, combining single variable domains, characterization of dual specific ligands, structure of dual specific ligands, scaffolds for use in constructing dual specific ligands, uses of anti-serum albumin dAbs and multispecific ligands and half-life-enhanced ligands, and compositions and formulations of comprising anti-serum albumin dAbs. These disclosures are incorporated herein by reference to provide guidance for use with the present invention, including for variants, ligands, fusion proteins, conjugates, nucleic acids, vectors, hosts and compositions of the present invention.

DOM7h-14 variant sequences, which are not according to the invention, are disclosed in a co-pending US provisional patent application entitled IMPROVED ANTI-SERUM ALBUMIN BINDING VARIANTS, filed on the same day as the present application. These sequences of DOM7h-14 variants (SEQ ID NO:s 1-10 in the co-pending application) are incorporated herein by reference as though explicitly written herein.

SEQUENCES

TABLE 1 Amino Acid Sequences of DOM7h-11 Variant dAbs DOM7h-11-12 (SEQ ID NO: 1) DIQMTQSPSSLSASVGDRVTITCRASRPIGTMLSWYQQKPGKAPKLLILF GSRLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQAGTHPTTFGQ GTKVEIKR DOM7h-11-15 (SEQ ID NO: 2) DIQMTQSPSSLSASVGDRVTITCRASRPIGTMLSWYQQKPGKAPKLLILA FSRLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQAGTHPTTFGQ GTKVEIKR DOM7h-11-18 (SEQ ID NO: 3) DIQMTQSPSSLSASVGDRVTITCRASRPIGTMLSWYQQKPGKAPKLLIWF GSRLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYHCAQAGTHPTTFGQ GTKVEIKR DOM7h-11-19 (SEQ ID NO: 4) DIQMTQSPSSLSASVGDRVTITCRASRPIGTMLSWYQQKPGKAPKLLILF GSRLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQTGTHPTTFGQ GTKVEIKR DOM7h-11-3 (SEQ ID NO: 5) DIQMTQSPSSLSASVGDRVTITCRASRPIGTTLSWYQQKPGKAPKLLILW NSRLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQAGTHPTTFGQ GTKVEIKR

TABLE 2 Nucleotide Sequences of DOM7h-11 Variant dAbs DOM7h-11-12 (SEQ ID NO: 6) GACATCCAGA TGACCCAGTC TCCATCCTCC CTGTCTGCAT CTGTAGGAGA CCGTGTCACC ATCACTTGCC GGGCAAGTCG TCCGATTGGG ACGATGTTAA GTTGGTACCA GCAGAAACCA GGGAAAGCCC CTAAGCTCCT GATCTTGTTT GGTTCCCGGT TGCAAAGTGG GGTCCCATCA CGTTTCAGTG GCAGTGGATC TGGGACAGAT TTCACTCTCA CCATCAGCAG TCTGCAACCT GAAGATTTTG CTACGTACTA CTGTGCGCAG GCTGGGACGC ATCCTACGAC GTTCGGCCAA GGGACCAAGG TGGAAATCAA ACGG DOM7h-11-15 (SEQ ID NO: 7) GACATCCAGA TGACCCAGTC TCCATCCTCC CTGTCTGCAT CTGTAGGAGA CCGTGTCACC ATCACTTGCC GGGCAAGTCG TCCGATTGGG ACGATGTTAA GTTGGTACCA GCAGAAACCA GGGAAAGCCC CTAAGCTCCT GATCCTTGCT TTTTCCCGTT TGCAAAGTGG GGTCCCATCA CGTTTCAGTG GCAGTGGATC TGGGACAGAT TTCACTCTCA CCATCAGCAG TCTGCAACCT GAAGATTTTG CTACGTACTA CTGCGCGCAG GCTGGGACGC ATCCTACGAC GTTCGGCCAA GGGACCAAGG TGGAAATCAA ACGG DOM7h-11-18 (SEQ ID NO: 8) GACATCCAGA TGACCCAGTC TCCATCCTCC CTGTCTGCAT CTGTAGGAGA CCGTGTCACC ATCACTTGCC GGGCAAGTCG TCCGATTGGG ACGATGTTAA GTTGGTACCA GCAGAAACCA GGGAAAGCCC CAAAGCTCCT GATCTGGTTT GGTTCCCGGT TGCAAAGTGG GGTCCCATCA CGTTTCAGTG GCAGTGGATC TGGGACAGAT TTCACTCTCA CCATCAGCAG TCTGCAACCT GAAGATTTTG CTACGTACCA CTGTGCGCAG GCGGGGACGC ATCCTACGAC GTTCGGCCAA GGGACCAAGG TGGAAATCAA ACGG DOM7h-11-19 (SEQ ID NO: 9) GACATCCAGA TGACCCAGTC TCCATCCTCC CTGTCTGCAT CTGTAGGAGA CCGTGTCACC ATCACTTGCC GGGCAAGTCG TCCGATTGGG ACGATGTTAA GTTGGTACCA GCAGAAACCA GGGAAAGCCC CTAAGCTCCT GATCTTGTTT GGTTCCCGGT TGCAAAGTGG GGTCCCATCA CGTTTCAGTG GCAGTGGATC TGGGACGGAT TTCACTCTCA CCATCAGCAG TCTGCAACCT GAAGATTTTG CTACGTACTA CTGTGCGCAG ACTGGGACGC ATCCCACGAC GTTCGGCCAA GGGACCAAGG TGGAAATCAA ACGG DOM7h-11-3 (SEQ ID NO: 10) GACATCCAGA TGACCCAGTC TCCATCCTCC CTGTCTGCAT CTGTAGGAGA CCGTGTCACC ATCACTTGCC GGGCAAGTCG TCCGATTGGG ACGACGTTAA GTTGGTACCA GCAGAAACCA GGGAAAGCCC CTAAGCTCCT GATCCTTTGG AATTCCCGTT TGCAAAGTGG GGTCCCATCA CGTTTCAGTG GCAGTGGATC TGGGACAGAT TTCACTCTCA CCATCAGCAG TCTGCAACCT GAAGATTTTG CTACGTACTA CTGTGCGCAG GCTGGGACGC ATCCTACGAC GTTCGGCCAA GGGACCAAGG TGGAAATCAA ACGG

TABLE 3 Amino Acid Sequences of anti-TNFR1 dAbs >DOM1h-509 (SEQ ID NO: 11) EVQLLESGGGLVQPGGSLRLSCAASGFTFSQYRMHWVRQAPGKSLEWVSSIDTRGSST YYADPVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAKAVTMFSPFFDYWGQGTLV TVSS >DOM1h-510 (SEQ ID NO: 12) EVQLLESGGGLVQPGGSLRLSCAASGFTFADYGMRWVRQAPGKGLEWVSSITRTGRVT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAKWRNRHGEYLADFDYWGQG TLVTVSS >DOM1h-543 (SEQ ID NO: 13) EVQLLESGGGLVQPGGSLRLSCAASGFTFMRYRMHWVRQAPGKGLEWVSSIDSNGSST YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAKDRTERSPVFDYWGQGTLV TVSS >DOM1h-549 (SEQ ID NO: 14) EVQLLESGGGLVQPGGSLRLSCAASGFTFVDYEMHWVRQAPGKGLEWVSSISESGTTT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAKRRFSASTFDYWGQGTLVT VSS >DOM1h-574 (SEQ ID NO: 15) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGGHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAKYTGHWEPFDYWGQGTLVT VSS >DOM1h-574-1 (SEQ ID NO: 16) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGGHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAKYTGRWEPYDYWGQGTLVT VSS >DOM1h-574-2 (SEQ ID NO: 17) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGGHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAKYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-7 (SEQ ID NO: 18) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGGHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-8 (SEQ ID NO: 19) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGPEWVSQISNTGGHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-9 (SEQ ID NO: 20) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGGHT YYADSVKGRFTISRDNSKNTLYMQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-10 (SEQ ID NO: 21) EVQLLESGGGLVQPGGSLRLSCAASGFTFGKYSMGWVRQAPGKDLEWVSQISNTGGHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-11 (SEQ ID NO: 22) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGGHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAKYTGRWEPFDHWGQGTLVT VSS >DOM1h-574-12 (SEQ ID NO: 23) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAKYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-13 (SEQ ID NO: 24) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAKYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-14 (SEQ ID NO: 25) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-15 (SEQ ID NO: 26) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-16 (SEQ ID NO: 27) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGPEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-17 (SEQ ID NO: 28) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGPEWVSQISNTGDHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-18 (SEQ ID NO: 29) EVQLLESGGGLVQPGGSLRLSCAASGFTFGKYSMGWVRQAPGKDLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-19 (SEQ ID NO: 30) EVQLLESGGGLVQPGGSLRLSCAASGFTFGKYSMGWVRQAPGKDLEWVSQISNTGDHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-25 (SEQ ID NO: 31) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-26 (SEQ ID NO: 32) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFEYWGQGTLVT VSS >DOM1h-574-27 (SEQ ID NO: 33) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWKPFEYWGQGTLVT VSS >DOM1h-574-28 (SEQ ID NO: 34) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-29 (SEQ ID NO: 35) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWRPFEYWGQGTLVT VSS >DOM1h-574-30 (SEQ ID NO: 36) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTGDRR YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAAYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-31 (SEQ ID NO: 37) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFNYWGQGTLVT VSS >DOM1h-574-32 (SEQ ID NO: 38) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-33 (SEQ ID NO: 39) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNSLYLQMNSLRAEDTAVYYCAIYTGRWVPFDNWGQGTLVT VSS >DOM1h-574-35 (SEQ ID NO: 40) EVQLLESGGGLVQPGGSLRLSCAASGFTFITYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFQYWGQGTLVT VSS >DOM1h-574-36 (SEQ ID NO: 41) EVQLLESGGGLVQPGGSLRLSCAASGFTFGKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-37 (SEQ ID NO: 42) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-38 (SEQ ID NO: 43) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-39 (SEQ ID NO: 44) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRR YYADAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-40 (SEQ ID NO: 45) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFKYWGQGTLVT VSS >DOM1h-574-53 (SEQ ID NO: 46) EVQLLESGGGLVQPGGSLRLSCAASGFTFSKYSMGWVRQAPGKGLEWVSQISNTGERR YYADSVKGRFTISRDNPKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFEYWGQGTLVT VSS >DOM1h-574-54 (SEQ ID NO: 47) EVQLLESGGGLVQPGGSLRLSCAASGFTFVNYSMGWVRQAPGKGLEWVSQISNTGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPYEYWGQGTLVT VTS >DOM1h-574-65 (SEQ ID NO: 48) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTGDRR YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-66 (SEQ ID NO: 49) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTGDRR YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWKPFEYWGQGTLVT VSS >DOM1h-574-67 (SEQ ID NO: 50) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTGDRR YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-68 (SEQ ID NO: 51) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTGDRR YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWRPFEYWGQGTLVT VSS >DOM1h-574-69 (SEQ ID NO: 52) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTGDRR YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-70 (SEQ ID NO: 53) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAVYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-71 (SEQ ID NO: 54) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWKPFEYWGQGTLVT VSS >DOM1h-574-72 (SEQ ID NO: 55) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-73 (SEQ ID NO: 56) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWRPFEYWGQGTLVT VSS >DOM1h-574-74 (SEQ ID NO: 57) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-75 (SEQ ID NO: 58) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-76 (SEQ ID NO: 59) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWKPFEYWGQGTLVT VSS >DOM1h-574-77 (SEQ ID NO: 60) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-78 (SEQ ID NO: 61) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWRPFEYWGQGTLVT VSS >DOM1h-574-79 (SEQ ID NO: 62) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-84 (SEQ ID NO: 63) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRR YYADAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-85 (SEQ ID NO: 64) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRR YYADAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWKPFEYWGQGTLVT VSS >DOM1h-574-86 (SEQ ID NO: 65) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRR YYADAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-87 (SEQ ID NO: 66) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRR YYADAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWRPFEYWGQGTLVT VSS >DOM1h-574-88 (SEQ ID NO: 67) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRR YYADAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-90 (SEQ ID NO: 68) EVQLLESGGGLVQPGGSLRLSCAASGFTFLKFSMGWVRQAPGKGLEWVSQIANTGDRR YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-91 (SEQ ID NO: 69) EVQLLESGGGLVQPGGSLRLSCAASGFTFLKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-92 (SEQ ID NO: 70) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-93 (SEQ ID NO: 71) EVQLLESGGGLVQPGGSLRLSCAASGFTFLKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-94 (SEQ ID NO: 72) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTGDRR YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAAYYCAIYTGRWPDFDYWGQGTLVT VSS >DOM1h-574-95 (SEQ ID NO: 73) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTGDRR YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAAYYCAIYTGRWPDFEYWGQGTLVT VSS >DOM1h-574-96 (SEQ ID NO: 74) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWPDFDYWGQGTLVT VSS >DOM1h-574-97 (SEQ ID NO: 75) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWPDFEYWGQGTLVT VSS >DOM1h-574-98 (SEQ ID NO: 76) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWPDFDYWGQGTLVT VSS >DOM1h-574-99 (SEQ ID NO: 77) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWPDFEYWGQGTLVT VSS >DOM1h-574-100 (SEQ ID NO: 78) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGPEWVSQISAWGDRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-101 (SEQ ID NO: 79) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGPEWVSQISDGGQRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-102 (SEQ ID NO: 80) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGPEWVSQISDSGYRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-103 (SEQ ID NO: 81) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGPEWVSQISDGGTRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-104 (SEQ ID NO: 82) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGPEWVSQISDKGTRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-105 (SEQ ID NO: 83) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGPEWVSQISETGRRT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-106 (SEQ ID NO: 84) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQINNTGSTT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFDYWGQGTLVT VSS >DOM1h-574-107 (SEQ ID NO: 85) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGPEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-108 (SEQ ID NO: 86) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGPEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-109 (SEQ ID NO: 87) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-110 (SEQ ID NO: 88) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-111 (SEQ ID NO: 89) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWRPFEYWGQGTLVT VSS >DOM1h-574-112 (SEQ ID NO: 90) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYTHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-113 (SEQ ID NO: 91) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRR YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-114 (SEQ ID NO: 92) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQILNTADRT YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-115 (SEQ ID NO: 93) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-116 (SEQ ID NO: 94) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRR YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-117 (SEQ ID NO: 95) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRR YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-118 (SEQ ID NO: 96) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAVYTGRWVSFEYWGQGTLVT VSS >DOM1h-574-119 (SEQ ID NO: 97) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCALYTGRWVSFEYWGQGTLVT VSS >DOM1h-574-120 (SEQ ID NO: 98) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAVYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-121 (SEQ ID NO: 99) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCALYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-122 (SEQ ID NO: 100) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTADRR YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-123 (SEQ ID NO: 101) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRR YYADAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-124 (SEQ ID NO: 102) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGDRR YYAHAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-125 (SEQ ID NO: 103) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTADRR YYADAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-126 (SEQ ID NO: 104) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTGDRR YYAHAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-127 (SEQ ID NO: 105) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTADRR YYAHAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-128 (SEQ ID NO: 106) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTADRR YYAHAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-129 (SEQ ID NO: 107) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIVNTGDRR YYADAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-130 (SEQ ID NO: 108) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIANTGDRR YYADAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-131 (SEQ ID NO: 109) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-132 (SEQ ID NO: 110) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWRPFEYWGQGTLVT VSS >DOM1h-574-133 (SEQ ID NO: 111) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-134 (SEQ ID NO: 112) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYSHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-135 (SEQ ID NO: 113) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYTHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-137 (SEQ ID NO: 114) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYTDAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-138 (SEQ ID NO: 115) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-139 (SEQ ID NO: 116) EVQLLESGGGLVQPGGSLRLSCAASGFTFLKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-140 (SEQ ID NO: 117) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQIADTGDRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-141 (SEQ ID NO: 118) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTADRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-142 (SEQ ID NO: 119) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-143 (SEQ ID NO: 120) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDDAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-144 (SEQ ID NO: 121) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQIADTADRR YYDDSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-145 (SEQ ID NO: 122) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQIADTGDRR YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-146 (SEQ ID NO: 123) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQIADTGDRR YYDDAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-147 (SEQ ID NO: 124) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWGPFVYWGQGTLVT VSS >DOM1h-574-14 8 (SEQ ID NO: 125) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFAYWGQGTLVT VSS >DOM1h-574-149 (SEQ ID NO: 126) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWGPFQYWGQGTLVT VSS >DOM1h-574-150 (SEQ ID NO: 127) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFQYWGQGTLVT VSS >DOM1h-574-151 (SEQ ID NO: 128) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-152 (SEQ ID NO: 129) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFQYWGQGTLVT VSS >DOM1h-574-153 (SEQ ID NO: 130) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFQYWGQGTLVT VSS >DOM1h-574-154 (SEQ ID NO: 131) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-155 (SEQ ID NO: 132) EVQLLESGGGLVQPGGSLRLSCAASGFTFLKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-156 (SEQ ID NO: 133) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-157 (SEQ ID NO: 134) EVQLLESGGGLVQPGGSLRLSCAASGFTFLKYSMGWVRQAPGKGLEWVSQISDTADRT YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWRPFEYWGQGTLVT VSS >DOM1h-574-158 (SEQ ID NO: 135) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTADRT YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWRPFEYWGQGTLVT VSS >DOM1h-574-159 (SEQ ID NO: 136) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTADRT YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-160 (SEQ ID NO: 137) EVQLLESGGGLVQPGGSLRLSCAASGFTFLKYSMGWVRQAPGKGLEWVSQISDTADRT YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-161 (SEQ ID NO: 138) EVQLLESGGGLVQPGGSLRLSCAASGFTFLKYSMGWVRQAPGKGLEWVSQISDTADRT YYSHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-162 (SEQ ID NO: 139) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTADRT YYSHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-163 (SEQ ID NO: 140) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTADRT YYTHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-164 (SEQ ID NO: 141) EVQLLESGGGLVQPGGSLRLSCAASGFTFLKYSMGWVRQAPGKGLEWVSQISDTADRT YYTHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-165 (SEQ ID NO: 142) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-166 (SEQ ID NO: 143) EVQLLESGGGLVQPGGSLRLSCAASGFTFLKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-167 (SEQ ID NO: 144) EVQLLESGGGLVQPGGSLRLSCAASGFTFLKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-169 (SEQ ID NO: 145) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIADTADRT YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-170 (SEQ ID NO: 146) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-171 (SEQ ID NO: 147) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIADTADRT YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-172 (SEQ ID NO: 148) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIADTADRT YYDHAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-173 (SEQ ID NO: 149) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIADTADRR YYAHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-174 (SEQ ID NO: 150) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRR YYAHAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-175 (SEQ ID NO: 151) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIADTADRR YYAHAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-176 (SEQ ID NO: 152) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRR YYDHAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-177 (SEQ ID NO: 153) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIADTADRR YYDHAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-178 (SEQ ID NO: 154) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQIADTADRR YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS >DOM1h-574-179 (SEQ ID NO: 155) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTADRR YYDDAVKGRFTITRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWEPFVYWGQGTLVT VSS >DOM1h-574-180 (SEQ ID NO: 156) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISDTADRT YYAHAVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWVPFEYWGQGTLVT VSS >DOM1h-574-4 (SEQ ID NO: 157) EVQLLESGGGLVQPGGSLRLSCAASGFTFVKYSMGWVRQAPGKGLEWVSQISNTGGHT YYADSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAKYTGRWEPFEYWGQGTLVT VSS >DOM1h-574-168 (SEQ ID NO: 158) EVQLLESGGGLVQPGGSLRLSCAASGFTFFKYSMGWVRQAPGKGLEWVSQISDTGDRR YYDHSVKGRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAIYTGRWAPFEYWGQGTLVT VSS

TABLE 4 Nucleotide sequences of anti-TNFR1 dAbs >DOM1h-509 (SEQ ID NO: 157) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTAGTCAGTATAGGATGCATTGGGTCCGCCA GGCTCCAGGGAAGAGTCTAGAGTGGGTCTCAAGTATTGATACTAGGGGTTCGTCTACA TACTACGCAGACCCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GAAAGCTGTGACGATGTTTTCTCCTTTTTTTGACTACTGGGGTCAGGGAACCCTGGTC ACCGTCTCGAGC >DOM1h-510 (SEQ ID NO: 158) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGCTGATTATGGGATGCGTTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCATCTATTACGCGGACTGGTCGTGTTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GAAATGGCGGAATCGGCATGGTGAGTATCTTGCTGATTTTGACTACTGGGGTCAGGGA ACCCTGGTCACCGTCTCGAGC >DOM1h-543 (SEQ ID NO: 159) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTATGAGGTATAGGATGCATTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCATCGATTGATTCTAATGGTTCTAGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GAAAGATCGTACGGAGCGTTCGCCGGTTTTTGACTACTGGGGTCAGGGAACCCTGGTC ACCGTCTCGAGC >DOM1h-549 (SEQ ID NO: 160) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTGCAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTGATTATGAGATGCATTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCATCTATTAGTGAGAGTGGTACGACGACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GAAACGTCGTTTTTCTGCTTCTACGTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574 (SEQ ID NO: 161) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGGTCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GAAATATACGGGTCATTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-1 (SEQ ID NO: 162) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGGTCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GAAATATACGGGTCGTTGGGAGCCTTATGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-2 (SEQ ID NO: 163) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGGTCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GAAATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-4 (SEQ ID NO: 164) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGGTCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GAAATATACGGGTCGTTGGGAGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-180 (SEQ ID NO: 165) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACGCGGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-7 (SEQ ID NO: 166) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGGTCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-8 (SEQ ID NO: 167) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGATGGGTCCGCCA GGCTCCAGGGAAAGGTCCAGAGTGGGTCTCACAGATTTCGAATACGGGTGGTCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACA GTCTCGAGC >DOM1h-574-9 (SEQ ID NO: 168) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGGTCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATATCCCGCGACAATTCCAAGAACA CGCTGTATATGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-10 (SEQ ID NO: 169) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGGTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGATCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGGTCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-11 (SEQ ID NO: 170) GAGGTGCAGCTGTTGGAGTCAGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGGTCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GAAATATACGGGTCGTTGGGAGCCTTTTGACCACTGGGGTCAGGGGACCCTGGTCACC GTCTCGAGC >DOM1h-574-12 (SEQ ID NO: 171) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GAAATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-13 (SEQ ID NO: 172) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GAAATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-14 (SEQ ID NO: 173) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-15 (SEQ ID NO: 174) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-16 (SEQ ID NO: 175) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGATGGGTCCGCCA GGCTCCAGGGAAAGGTCCAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACA GTCTCGAGC >DOM1h-574-17 (SEQ ID NO: 176) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGATGGGTCCGCCA GGCTCCAGGGAAAGGTCCAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACA GTCTCGAGC >DOM1h-574-18 (SEQ ID NO: 177) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGGTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGATCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-19 (SEQ ID NO: 178) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGGTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGATCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCATACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-25 (SEQ ID NO: 179) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-26 (SEQ ID NO: 180) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-27 (SEQ ID NO: 181) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCGGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAAGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-28 (SEQ ID NO: 182) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-29 (SEQ ID NO: 183) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAGGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-30 (SEQ ID NO: 184) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGGTGATCGTAGA TACTACGCAGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGCATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-31 (SEQ ID NO: 185) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTAACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-32 (SEQ ID NO: 186) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-33 (SEQ ID NO: 187) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACT CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGTGCCTTTTGACAACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-35 (SEQ ID NO: 188) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTATTACGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTCAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-36 (SEQ ID NO: 189) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGGTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCGGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-37 (SEQ ID NO: 190) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAAGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-38 (SEQ ID NO: 191) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-39 (SEQ ID NO: 192) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTAGA TACTACGCAGACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-40 (SEQ ID NO: 193) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTAAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-53 (SEQ ID NO: 194) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTAGTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGAGCGTAGA TACTACGCAGACTCAGTGAAGGGCCGGTTCACCATCTCCCGCGACAATCCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGAGCCTTTTGAATACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-54 (SEQ ID NO: 195) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAACTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTACA TACTACGCGGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTATGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCACGAGC >DOM1h-574-65 (SEQ ID NO: 196) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGGTGATCGTAGA TACTACGCAGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGATAATTCCAAGAACA CACTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-66 (SEQ ID NO: 197) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGGTGATCGTAGA TACTACGCAGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAAGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-67 (SEQ ID NO: 198) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGGTGATCGTAGA TACTACGCAGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-68 (SEQ ID NO: 199) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGGTGATCGTAGA TACTACGCAGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAGGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-69 (SEQ ID NO: 200) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGGTGATCGTAGA TACTACGCAGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-70 (SEQ ID NO: 201) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GGTATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-71 (SEQ ID NO: 202) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAAGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-72 (SEQ ID NO: 203) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-73 (SEQ ID NO: 204) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAGGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-74 (SEQ ID NO: 205) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-75 (SEQ ID NO: 206) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-76 (SEQ ID NO: 207) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCCCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAAGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-77 (SEQ ID NO: 208) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-78 (SEQ ID NO: 209) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAGGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-79 (SEQ ID NO: 210) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-84 (SEQ ID NO: 211) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTAGA TACTACGCAGACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-85 (SEQ ID NO: 212) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTAGA TACTACGCAGACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAAGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-86 (SEQ ID NO: 213) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCCCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTAGA TACTACGCAGACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAAGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-87 (SEQ ID NO: 214) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTAGA TACTACGCAGACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAGGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-88 (SEQ ID NO: 215) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGTGATCGTAGA TACTACGCAGACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-90 (SEQ ID NO: 216) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTGAAGTTTTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGGTGATCGTAGA TACTACGCAGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-91 (SEQ ID NO: 217) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTGAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-92 (SEQ ID NO: 218) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-93 (SEQ ID NO: 219) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTGAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-94 (SEQ ID NO: 220) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGGTGATCGTAGA TACTACGCAGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGCATATTACTGTGC GATATATACGGGTCGGTGGCCCGACTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-95 (SEQ ID NO: 221) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGGTGATCGTAGA TACTACGCAGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGCATATTACTGTGC GATATATACGGGTCGGTGGCCCGACTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-96 (SEQ ID NO: 222) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGCCCGACTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-97 (SEQ ID NO: 223) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGCCCGACTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-98 (SEQ ID NO: 224) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGCCCGACTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-99 (SEQ ID NO: 225) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGCCCGACTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-100 (SEQ ID NO: 226) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGATGGGTCCGCCA GGCTCCAGGGAAAGGTCCAGAGTGGGTCTCACAGATTTCGGCCTGGGGTGACAGGACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-101 (SEQ ID NO: 227) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAAGGTCCAGAGTGGGTCTCACAGATTTCGGACGGCGGTCAGAGGACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-102 (SEQ ID NO: 228) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGATGGGTCCGCCA GGCTCCAGGGAAAGGTCCAGAGTGGGTCTCACAGATTTCGGACTCCGGTTACCGCACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-103 (SEQ ID NO: 229) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCCAGAGTGGGTCTCACAGATTTCGGACGGGGGTACGCGGACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-104 (SEQ ID NO: 230) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGATGGGTCCGCCA GGCTCCAGGGAAAGGTCCAGAGTGGGTCTCACAGATTTCGGACAAGGGTACGCGCACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-105 (SEQ ID NO: 231) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGATGGGTCCGCCA GGCTCCAGGGAAAGGTCCAGAGTGGGTCTCACAGATTTCGGAGACCGGTCGCAGGACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-106 (SEQ ID NO: 232) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTAACAATACGGGTTCGACCACA TACTACGCAGACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGACTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-107 (SEQ ID NO: 233) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCCAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-108 (SEQ ID NO: 234) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCCAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-109 (SEQ ID NO: 235) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-110 (SEQ ID NO: 236) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-111 (SEQ ID NO: 237) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAGGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-112 (SEQ ID NO: 238) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACACACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-113 (SEQ ID NO: 239) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGCAGA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-114 (SEQ ID NO: 240) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTTGAATACTGCTGATCGTACA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-115 (SEQ ID NO: 241) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-116 (SEQ ID NO: 242) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTAGA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-117 (SEQ ID NO: 243) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTAGA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-118 (SEQ ID NO: 244) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GGTATATACTGGGCGTTGGGTGTCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-119 (SEQ ID NO: 245) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GCTATATACTGGGCGTTGGGTGTCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-120 (SEQ ID NO: 246) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTTACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GGTATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-121 (SEQ ID NO: 247) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GCTATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-122 (SEQ ID NO: 248) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACTGCTGATCGTAGA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-123 (SEQ ID NO: 249) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTAGA TACTACGCAGACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-124 (SEQ ID NO: 250) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCGGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACGGGCGATCGTAGA TACTACGCACACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-125 (SEQ ID NO: 251) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACTGCTGATCGTAGA TACTACGCAGACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-126 (SEQ ID NO: 252) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGGTGATCGTAGA TACTACGCACACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-127 (SEQ ID NO: 253) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGAATACTGCTGATCGTAGA TACTACGCACACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-128 (SEQ ID NO: 254) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGCTGATCGTAGA TACTACGCACACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-129 (SEQ ID NO: 255) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGTGAATACGGGTGATCGTAGA TACTACGCAGACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-130 (SEQ ID NO: 256) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGAATACGGGTGATCGTAGA TACTACGCAGACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-131 (SEQ ID NO: 257) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-132 (SEQ ID NO: 258) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAGGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-133 (SEQ ID NO: 259) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-134 (SEQ ID NO: 260) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACTCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-135 (SEQ ID NO: 261) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACACACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-137 (SEQ ID NO: 262) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACACAGACGCGGTGAAGGGGCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-138 (SEQ ID NO: 263) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-139 (SEQ ID NO: 264) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTGAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-140 (SEQ ID NO: 265) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGGATACGGGTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-141 (SEQ ID NO: 266) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-142 (SEQ ID NO: 267) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGCC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATCACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAACCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-143 (SEQ ID NO: 268) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACGGGTGATCGTAGA TACTACGATGACGCGGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-144 (SEQ ID NO: 269) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGGATACTGCTGATCGTAGA TACTACGATGACTCTGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-145 (SEQ ID NO: 270) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGGATACGGGTGATCGTAGA TACTACGATCACTCTGTGAAGGGCCGGTTCACTATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-146 (SEQ ID NO: 271) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGGATACGGGTGATCGTAGA TACTACGATGACGCGGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-147 (SEQ ID NO: 272) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGGGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-14 8 (SEQ ID NO: 273) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGTGCCTTTTGCCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-149 (SEQ ID NO: 274) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGGACCTTTTCAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-150 (SEQ ID NO: 275) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTCAGTACTGGGGTCAGGGAACTCTGGTCACC GTCTCGAGC >DOM1h-574-151 (SEQ ID NO: 276) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-152 (SEQ ID NO: 277) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGCGCCTTTTCAGTACTGGGGTCAGGGAACTCTGGTCACC GTCTCGAGC >DOM1h-574-153 (SEQ ID NO: 278) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGTGCCTTTTCAGTACTGGGGTCAGGGCACCCTGGTCACC GTCTCGAGC >DOM1h-574-154 (SEQ ID NO: 279) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACCGGTGATCGTAGA TACTACGATCACTCTGTGAAGGGCCGGTTCACTATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-155 (SEQ ID NO: 280) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTGAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-156 (SEQ ID NO: 281) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-157 (SEQ ID NO: 282) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTGAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAGGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-158 (SEQ ID NO: 283) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGAGGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-159 (SEQ ID NO: 284) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-160 (SEQ ID NO: 285) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTGAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-161 (SEQ ID NO: 286) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTGAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACTCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-162 (SEQ ID NO: 287) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACTCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-163 (SEQ ID NO: 288) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACACACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-164 (SEQ ID NO: 289) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTGAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACACACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-165 (SEQ ID NO: 290) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-166 (SEQ ID NO: 291) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTGAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-167 (SEQ ID NO: 292) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTGAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACCGGTGATCGTAGA TACTACGATCACTCTGTGAAGGGCCGGTTCACTATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-168 (SEQ ID NO: 293) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACCGGTGATCGTAGA TACTACGATCACTCTGTGAAGGGCCGGTTCACTATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-169 (SEQ ID NO: 294) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGGATACTGCTGATCGTACA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGCGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-170 (SEQ ID NO: 295) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTACA TACTACGCACACGCGGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-171 (SEQ ID NO: 296) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTGCAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGGATACTGCTGATCGTACA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-172 (SEQ ID NO: 297) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGGATACTGCTGATCGTACA TACTACGATCACGCGGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCTGAGGACACCGCGGTATATTACTGTGC GATATATACTGGGCGTTGGGTGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-173 (SEQ ID NO: 298) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGGATACTGCTGATCGTAGA TACTACGCACACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-174 (SEQ ID NO: 299) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTAGA TACTACGCACACGCGGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-175 (SEQ ID NO: 300) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGGATACTGCTGATCGTAGA TACTACGCACACGCGGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-176 (SEQ ID NO: 301) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTAGA TACTACGATCACGCGGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-177 (SEQ ID NO: 302) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGGATACTGCTGATCGTAGA TACTACGATCACGCGGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGGACCCTGGTCACC GTCTCGAGC >DOM1h-574-178 (SEQ ID NO: 303) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTGTTAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTGCGGATACTGCTGATCGTAGA TACTACGATCACTCCGTGAAGGGCCGGTTCACCATCTCCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGGTGGGCGCCTTTTGAGTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC >DOM1h-574-179 (SEQ ID NO: 304) GAGGTGCAGCTGCTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCCCTGCGTC TCTCCTGTGCAGCCTCCGGATTCACCTTTTTCAAGTATTCGATGGGGTGGGTCCGCCA GGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACAGATTTCGGATACTGCTGATCGTAGA TACTACGATGACGCGGTGAAGGGCCGGTTCACCATCACCCGCGACAATTCCAAGAACA CGCTGTATCTGCAAATGAACAGCCTGCGTGCCGAGGACACCGCGGTATATTACTGTGC GATATATACGGGTCGTTGGGAGCCTTTTGTCTACTGGGGTCAGGGAACCCTGGTCACC GTCTCGAGC

TABLE 5 Anti-serum albumin dAb (DOM7h) fusions (used in Rat studies):- DOM7h-14/Exendin-4 fusion DMS number 7138 Amino acid sequence (SEQ ID NO: 305) HGEGTFTSDLSKQMEEEAVRLFIEWLKNGGPSSGAPPPSGGGGGSGGGGSG GGGSDIQMTQSPSSLSASVGDRVTITCRASQWIGSQLSWYQQKPGKAPKLL IMWRSSLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQGAALPRTF GQGTKVEIKR Nucleotide sequence (SEQ ID NO: 306) CATGGTGAAGGAACATTTACCAGTGACTTGTCAAAACAGATGGAAGAGGAG GCAGTGCGGTTATTTATTGAGTGGCTTAAGAACGGAGGACCAAGTAGCGGG GCACCTCCGCCATCGGGTGGTGGAGGCGGTTCAGGCGGAGGTGGCAGCGGC GGTGGCGGGTCGGACATCCAGATGACCCAGTCTCCATCCTCCCTGTCTGCA TCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGTCAGTGGATTGGG TCTCAGTTATCTTGGTACCAGCAGAAACCAGGGAAAGCCCCTAAGCTCCTG ATCATGTGGCGTTCCTCGTTGCAAAGTGGGGTCCCATCACGTTTCAGTGGC AGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGTCTGCAACCTGAA GATTTTGCTACGTACTACTGTGCTCAGGGTGCGGCGTTGCCTAGGACGTTC GGCCAAGGGACCAAGGTGGAAATCAAACGG DOM7h-14-10/Exendin-4 fusion DMS number 7139 Amino acid sequence (SEQ ID NO: 307) HGEGTFTSDLSKQMEEEAVRLFIEWLKNGGPSSGAPPPSGGGGGSGGGGSG GGGSDIQMTQSPSSLSASVGDRVTITCRASQWIGSQLSWYQQKPGKAPKLL IMWRSSLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQGLRHPKTF GQGTKVEIKR Nucleotide sequence (SEQ ID NO: 308) CATGGTGAAGGAACATTTACCAGTGACTTGTCAAAACAGATGGAAGAGGAG GCAGTGCGGTTATTTATTGAGTGGCTTAAGAACGGAGGACCAAGTAGCGGG GCACCTCCGCCATCGGGTGGTGGAGGCGGTTCAGGCGGAGGTGGCAGCGGC GGTGGCGGGTCGGACATCCAGATGACCCAGTCTCCATCCTCCCTGTCTGCA TCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGTCAGTGGATTGGG TCTCAGTTATCTTGGTACCAGCAGAAACCAGGGAAAGCCCCTAAGCTCCTG ATCATGTGGCGTTCCTCGTTGCAAAGTGGGGTCCCATCACGTTTCAGTGGC AGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGTCTGCAACCTGAA GATTTTGCTACGTACTACTGTGCTCAGGGTTTGAGGCATCCTAAGACGTTC GGCCAAGGGACCAAGGTGGAAATCAAACGG DOM7h-14-18/Exendin-4 fusion DMS number 7140 Amino acid sequence (SEQ ID NO: 309) HGEGTFTSDLSKQMEEEAVRLFIEWLKNGGPSSGAPPPSGGGGGSGGGGSG GGGSDIQMTQSPSSLSASVGDRVTITCRASQWIGSQLSWYQQKPGKAPKLL IMWRSSLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQGLMKPMTF GQGTKVEIKR Nucleotide sequence (SEQ ID NO: 310) CATGGTGAAGGAACATTTACCAGTGACTTGTCAAAACAGATGGAAGAGGAG GCAGTGCGGTTATTTATTGAGTGGCTTAAGAACGGAGGACCAAGTAGCGGG GCACCTCCGCCATCGGGTGGTGGAGGCGGTTCAGGCGGAGGTGGCAGCGGC GGTGGCGGGTCGGACATCCAGATGACCCAGTCTCCATCCTCCCTGTCTGCA TCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGTCAGTGGATTGGG TCTCAGTTATCTTGGTACCAGCAGAAACCAGGGAAAGCCCCTAAGCTCCTG ATCATGTGGCGTTCCTCGTTGCAAAGTGGGGTCCCATCACGTTTCAGTGGC AGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGTCTGCAACCTGAA GATTTTGCTACGTACTACTGTGCTCAGGGTCTTATGAAGCCTATGACGTTC GGCCAAGGGACCAAGGTGGAAATCAAACGG DOM7h-14-19/Exendin-4 fusion DMS number 7141 Amino acid sequence (SEQ ID NO: 311) HGEGTFTSDLSKQMEEEAVRLFIEWLKNGGPSSGAPPPSGGGGGSGGGGSG GGGSDIQMTQSPSSLSASVGDRVTISCRASQWIGSQLSWYQQKPGEAPKLL IMWRSSLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQGAALPRTF GQGTKVEIKR Nucleotide sequence (SEQ ID NO: 312) CATGGTGAAGGAACATTTACCAGTGACTTGTCAAAACAGATGGAAGAGGAG GCAGTGCGGTTATTTATTGAGTGGCTTAAGAACGGAGGACCAAGTAGCGGG GCACCTCCGCCATCGGGTGGTGGAGGCGGTTCAGGCGGAGGTGGCAGCGGC GGTGGCGGGTCGGACATCCAGATGACCCAGTCTCCATCCTCCCTGTCTGCA TCTGTAGGAGACCGTGTCACCATCTCTTGCCGGGCAAGTCAGTGGATTGGG TCTCAGTTATCTTGGTACCAGCAGAAACCAGGGGAAGCCCCTAAGCTCCTG ATCATGTGGCGTTCCTCGTTGCAAAGTGGGGTCCCATCACGTTTCAGTGGC AGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGTCTGCAACCTGAA GATTTTGCTACGTACTACTGTGCTCAGGGTGCGGCGTTGCCTAGGACGTTC GGCCAAGGGACCAAGGTGGAAATCAAACGG DOM7h-11/Exendin-4 fusion DMS number 7142 Amino acid sequence (SEQ ID NO: 313) HGEGTFTSDLSKQMEEEAVRLFIEWLKNGGPSSGAPPPSGGGGGSGGGGSG GGGSDIQMTQSPSSLSASVGDRVTITCRASRPIGTTLSWYQQKPGKAPKLL IWFGSRLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQAGTHPTTF GQGTKVEIKR Nucleotide sequence (SEQ ID NO: 314) CATGGTGAAGGAACATTTACCAGTGACTTGTCAAAACAGATGGAAGAGGAG GCAGTGCGGTTATTTATTGAGTGGCTTAAGAACGGAGGACCAAGTAGCGGG GCACCTCCGCCATCGGGTGGTGGAGGCGGTTCAGGCGGAGGTGGCAGCGGC GGTGGCGGGTCGGACATCCAGATGACCCAGTCTCCATCCTCCCTGTCTGCA TCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGTCGTCCGATTGGG ACGACGTTAAGTTGGTACCAGCAGAAACCAGGGAAAGCCCCTAAGCTCCTG ATCTGGTTTGGTTCCCGGTTGCAAAGTGGGGTCCCATCACGTTTCAGTGGC AGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGTCTGCAACCTGAA GATTTTGCTACGTACTACTGTGCGCAGGCTGGGACGCATCCTACGACGTTC GGCCAAGGGACCAAGGTGGAAATCAAACGG DOM7h-11-12/Exendin-4 fusion DMS number 7147 Amino acid sequence (SEQ ID NO: 315) HGEGTFTSDLSKQMEEEAVRLFIEWLKNGGPSSGAPPPSGGGGGSGGGGSG GGGSDIQMTQSPSSLSASVGDRVTITCRASRPIGTMLSWYQQKPGKAPKLL ILFGSRLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQAGTHPTTF GQGTKVEIKR Nucleotide sequence (SEQ ID NO: 316) CATGGTGAAGGAACATTTACCAGTGACTTGTCAAAACAGATGGAAGAGGAG GCAGTGCGGTTATTTATTGAGTGGCTTAAGAACGGAGGACCAAGTAGCGGG GCACCTCCGCCATCGGGTGGTGGAGGCGGTTCAGGCGGAGGTGGCAGCGGC GGTGGCGGGTCGGACATCCAGATGACCCAGTCTCCATCCTCCCTGTCTGCA TCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGTCGTCCGATTGGG ACGATGTTAAGTTGGTACCAGCAGAAACCAGGGAAAGCCCCTAAGCTCCTG ATCTTGTTTGGTTCCCGGTTGCAAAGTGGGGTCCCATCACGTTTCAGTGGC AGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGTCTGCAACCTGAA GATTTTGCTACGTACTACTGTGCGCAGGCTGGGACGCATCCTACGACGTTC GGCCAAGGGACCAAGGTGGAAATCAAACGG DOM7h-11-15/Exendin-4 fusion DMS number 7143 Amino acid sequence (SEQ ID NO: 317) HGEGTFTSDLSKQMEEEAVRLFIEWLKNGGPSSGAPPPSGGGGGSGGGGSG GGGSDIQMTQSPSSLSASVGDRVTITCRASRPIGTMLSWYQQKPGKAPKLL ILAFSRLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQAGTHPTTF GQGTKVEIKR Nucleotide sequence (SEQ ID NO: 318) CATGGTGAAGGAACATTTACCAGTGACTTGTCAAAACAGATGGAAGAGGAG GCAGTGCGGTTATTTATTGAGTGGCTTAAGAACGGAGGACCAAGTAGCGGG GCACCTCCGCCATCGGGTGGTGGAGGCGGTTCAGGCGGAGGTGGCAGCGGC GGTGGCGGGTCGGACATCCAGATGACCCAGTCTCCATCCTCCCTGTCTGCA TCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGTCGTCCGATTGGG ACGATGTTAAGTTGGTACCAGCAGAAACCAGGGAAAGCCCCTAAGCTCCTG ATCCTTGCTTTTTCCCGTTTGCAAAGTGGGGTCCCATCACGTTTCAGTGGC AGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGTCTGCAACCTGAA GATTTTGCTACGTACTACTGCGCGCAGGCTGGGACGCATCCTACGACGTTC GGCCAAGGGACCAAGGTGGAAATCAAACGG DOM7h14-10/G4SC-NCE fusion Amino acid sequence (SEQ ID NO: 319) encoding DOM7h14-10/G4SC DIQMTQSPSSLSASVGDRVTITCRASQWIGSQLSWYQQKPGKAPKLLIMWR SSLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQGLRHPKTFGQGT KVEIKRGGGGSC The C-terminal cysteine can be linked to a new chemical entity (pharmaceutical chemical compound, NCE), eg using maleimide linkage. Nucleotide sequence (SEQ ID NO: 320) encoding DOM7h14-10/G4SC GACATCCAGATGACCCAGTCTCCATCCTCCCTGTCTGCATCTGTAGGAGAC CGTGTCACCATCACTTGCCGGGCAAGTCAGTGGATTGGGTCTCAGTTATCT TGGTACCAGCAGAAACCAGGGAAAGCCCCTAAGCTCCTGATCATGTGGCGT TCCTCGTTGCAAAGTGGGGTCCCATCACGTTTCAGTGGCAGTGGATCTGGG ACAGATTTCACTCTCACCATCAGCAGTCTGCAACCTGAAGATTTTGCTACG TACTACTGTGCTCAGGGTTTGAGGCATCCTAAGACGTTCGGCCAAGGGACC AAGGTGGAAATCAAACGGGGTGGCGGAGGGGGTTCCTGT DOM7h14-10/TVAAPSC fusion Amino acid sequence (SEQ ID NO: 321) DIQMTQSPSSLSASVGDRVTITCRASQWIGSQLSWYQQKPGKAPKLLIMWR SSLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQGLRHPKTFGQGT KVEIKRTVAAPSC The C-terminal cysteine can be linked to a new chemical entity (pharmaceutical chemical compound, NCE), eg using maleimide linkage. Nucleotide sequence (SEQ ID NO: 322) GACATCCAGATGACCCAGTCTCCATCCTCCCTGTCTGCATCTGTAGGAGAC CGTGTCACCATCACTTGCCGGGCAAGTCAGTGGATTGGGTCTCAGTTATCT TGGTACCAGCAGAAACCAGGGAAAGCCCCTAAGCTCCTGATCATGTGGCGT TCCTCGTTGCAAAGTGGGGTCCCATCACGTTTCAGTGGCAGTGGATCTGGG ACAGATTTCACTCTCACCATCAGCAGTCTGCAACCTGAAGATTTTGCTACG TACTACTGTGCTCAGGGTTTGAGGCATCCTAAGACGTTCGGCCAAGGGACC AAGGTGGAAATCAAACGGACCGTCGCTGCTCCATCTTGT (used in mouse studies):- DOM7h-11/DOM1m-21-23 fusion DMS number 5515 Amino acid sequence (SEQ ID NO: 323) EVQLLESGGGLVQPGGSLRLSCAASGFTFNRYSMGWLRQAPGKGLEWVSRI DSYGRGTYYEDPVKGRFSISRDNSKNTLYLQMNSLRAEDTAVYYCAKISQF GSNAFDYWGQGTQVTVSSASTSGPSDIQMTQSPSSLSASVGDRVTITCRAS RPIGTTLSWYQQKPGKAPKLLIWFGSRLQSGVPSRFSGSGSGTDFTLTISS LQPEDFATYYCAQAGTHPTTFGQGTKVEIKR Amino acid plus nucleotide plus myc tag sequence (SEQ ID NO: 324) EVQLLESGGGLVQPGGSLRLSCAASGFTFNRYSMGWLRQAPGKGLEWVSRI DSYGRGTYYEDPVKGRFSISRDNSKNTLYLQMNSLRAEDTAVYYCAKISQF GSNAFDYWGQGTQVTVSSASTSGPSDIQMTQSPSSLSASVGDRVTITCRAS RPIGTTLSWYQQKPGKAPKLLIWFGSRLQSGVPSRFSGSGSGTDFTLTISS LQPEDFATYYCAQAGTHPTTFGQGTKVEIKRAAAEQKLISEEDLN Nucleotide sequence (SEQ ID NO: 325) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCC CTGCGTCTCTCCTGTGCAGCCTCCGGATTCACCTTTAATAGGTATAGTATG GGGTGGCTCCGCCAGGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACGGATT GATTCTTATGGTCGTGGTACATACTACGAAGACCCCGTGAAGGGCCGGTTC AGCATCTCCCGCGACAATTCCAAGAACACGCTGTATCTGCAAATGAACAGC CTGCGTGCCGAGGACACCGCCGTATATTACTGTGCGAAAATTTCTCAGTTT GGGTCAAATGCGTTTGACTACTGGGGTCAGGGAACCCAGGTCACCGTCTCG AGCGCTAGCACCAGTGGTCCATCGGACATCCAGATGACCCAGTCTCCATCC TCCCTGTCTGCATCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGT CGTCCGATTGGGACGACGTTAAGTTGGTACCAGCAGAAACCAGGGAAAGCC CCTAAGCTCCTGATCTGGTTTGGTTCCCGGTTGCAAAGTGGGGTCCCATCA CGTTTCAGTGGCAGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGT CTGCAACCTGAAGATTTTGCTACGTACTACTGTGCGCAGGCTGGGACGCAT CCTACGACGTTCGGCCAAGGGACCAAGGTGGAAATCAAACGG Nucleotide plus myc tag sequence (SEQ ID NO: 326) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCC CTGCGTCTCTCCTGTGCAGCCTCCGGATTCACCTTTAATAGGTATAGTATG GGGTGGCTCCGCCAGGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACGGATT GATTCTTATGGTCGTGGTACATACTACGAAGACCCCGTGAAGGGCCGGTTC AGCATCTCCCGCGACAATTCCAAGAACACGCTGTATCTGCAAATGAACAGC CTGCGTGCCGAGGACACCGCCGTATATTACTGTGCGAAAATTTCTCAGTTT GGGTCAAATGCGTTTGACTACTGGGGTCAGGGAACCCAGGTCACCGTCTCG AGCGCTAGCACCAGTGGTCCATCGGACATCCAGATGACCCAGTCTCCATCC TCCCTGTCTGCATCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGT CGTCCGATTGGGACGACGTTAAGTTGGTACCAGCAGAAACCAGGGAAAGCC CCTAAGCTCCTGATCTGGTTTGGTTCCCGGTTGCAAAGTGGGGTCCCATCA CGTTTCAGTGGCAGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGT CTGCAACCTGAAGATTTTGCTACGTACTACTGTGCGCAGGCTGGGACGCAT CCTACGACGTTCGGCCAAGGGACCAAGGTGGAAATCAAACGGGCGGCCGCA GAACAAAAACTCATCTCAGAAGAGGATCTGAATTAA DOM7h-11-12/DOM1m-21-23 fusion DMS number 5516 Amino acid sequence (SEQ ID NO: 327) EVQLLESGGGLVQPGGSLRLSCAASGFTFNRYSMGWLRQAPGKGLEWVSRI DSYGRGTYYEDPVKGRFSISRDNSKNTLYLQMNSLRAEDTAVYYCAKISQF GSNAFDYWGQGTQVTVSSASTSGPSDIQMTQSPSSLSASVGDRVTITCRAS RPIGTMLSWYQQKPGKAPKLLILFGSRLQSGVPSRFSGSGSGTDFTLTISS LQPEDFATYYCAQAGTHPTTFGQGTKVEIKR Amino acid plus nucleotide plus myc tag sequence (SEQ ID NO: 328) EVQLLESGGGLVQPGGSLRLSCAASGFTFNRYSMGWLRQAPGKGLEWVSRI DSYGRGTYYEDPVKGRFSISRDNSKNTLYLQMNSLRAEDTAVYYCAKISQF GSNAFDYWGQGTQVTVSSASTSGPSDIQMTQSPSSLSASVGDRVTITCRAS RPIGTMLSWYQQKPGKAPKLLILFGSRLQSGVPSRFSGSGSGTDFTLTISS LQPEDFATYYCAQAGTHPTTFGQGTKVEIKRAAAEQKLISEEDLN Nucleotide sequence (SEQ ID NO: 329) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCC CTGCGTCTCTCCTGTGCAGCCTCCGGATTCACCTTTAATAGGTATAGTATG GGGTGGCTCCGCCAGGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACGGATT GATTCTTATGGTCGTGGTACATACTACGAAGACCCCGTGAAGGGCCGGTTC AGCATCTCCCGCGACAATTCCAAGAACACGCTGTATCTGCAAATGAACAGC CTGCGTGCCGAGGACACCGCCGTATATTACTGTGCGAAAATTTCTCAGTTT GGGTCAAATGCGTTTGACTACTGGGGTCAGGGAACCCAGGTCACCGTCTCG AGCGCTAGCACCAGTGGTCCATCGGACATCCAGATGACCCAGTCTCCATCC TCCCTGTCTGCATCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGT CGTCCGATTGGGACGATGTTAAGTTGGTACCAGCAGAAACCAGGGAAAGCC CCTAAGCTCCTGATCTTGTTTGGTTCCCGGTTGCAAAGTGGGGTCCCATCA CGTTTCAGTGGCAGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGT CTGCAACCTGAAGATTTTGCTACGTACTACTGTGCGCAGGCTGGGACGCAT CCTACGACGTTCGGCCAAGGGACCAAGGTGGAAATCAAACGG Nucleotide plus myc tag sequence (SEQ ID NO: 330) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCC CTGCGTCTCTCCTGTGCAGCCTCCGGATTCACCTTTAATAGGTATAGTATG GGGTGGCTCCGCCAGGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACGGATT GATTCTTATGGTCGTGGTACATACTACGAAGACCCCGTGAAGGGCCGGTTC AGCATCTCCCGCGACAATTCCAAGAACACGCTGTATCTGCAAATGAACAGC CTGCGTGCCGAGGACACCGCCGTATATTACTGTGCGAAAATTTCTCAGTTT GGGTCAAATGCGTTTGACTACTGGGGTCAGGGAACCCAGGTCACCGTCTCG AGCGCTAGCACCAGTGGTCCATCGGACATCCAGATGACCCAGTCTCCATCC TCCCTGTCTGCATCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGT CGTCCGATTGGGACGATGTTAAGTTGGTACCAGCAGAAACCAGGGAAAGCC CCTAAGCTCCTGATCTTGTTTGGTTCCCGGTTGCAAAGTGGGGTCCCATCA CGTTTCAGTGGCAGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGT CTGCAACCTGAAGATTTTGCTACGTACTACTGTGCGCAGGCTGGGACGCAT CCTACGACGTTCGGCCAAGGGACCAAGGTGGAAATCAAACGGGCGGCCGCA GAACAAAAACTCATCTCAGAAGAGGATCTGAATTAA DOM7h-11-15/DOM1m-21-23 fusion DMS number 5517 Amino acid sequence (SEQ ID NO: 331) EVQLLESGGGLVQPGGSLRLSCAASGFTFNRYSMGWLRQAPGKGLEWVSRI DSYGRGTYYEDPVKGRFSISRDNSKNTLYLQMNSLRAEDTAVYYCAKISQF GSNAFDYWGQGTQVTVSSASTSGPSDIQMTQSPSSLSASVGDRVTITCRAS RPIGTMLSWYQQKPGKAPKLLILAFSRLQSGVPSRFSGSGSGTDFTLTISS LQPEDFATYYCAQAGTHPTTFGQGTKVEIKR Amino acid plus nucleotide plus myc tag sequence (SEQ ID NO: 332) EVQLLESGGGLVQPGGSLRLSCAASGFTFNRYSMGWLRQAPGKGLEWVSRI DSYGRGTYYEDPVKGRFSISRDNSKNTLYLQMNSLRAEDTAVYYCAKISQF GSNAFDYWGQGTQVTVSSASTSGPSDIQMTQSPSSLSASVGDRVTITCRAS RPIGTMLSWYQQKPGKAPKLLILAFSRLQSGVPSRFSGSGSGTDFTLTISS LQPEDFATYYCAQAGTHPTTFGQGTKVEIKRAAAEQKLISEEDLN Nucleotide sequence (SEQ ID NO: 333) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCC CTGCGTCTCTCCTGTGCAGCCTCCGGATTCACCTTTAATAGGTATAGTATG GGGTGGCTCCGCCAGGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACGGATT GATTCTTATGGTCGTGGTACATACTACGAAGACCCCGTGAAGGGCCGGTTC AGCATCTCCCGCGACAATTCCAAGAACACGCTGTATCTGCAAATGAACAGC CTGCGTGCCGAGGACACCGCCGTATATTACTGTGCGAAAATTTCTCAGTTT GGGTCAAATGCGTTTGACTACTGGGGTCAGGGAACCCAGGTCACCGTCTCG AGCGCTAGCACCAGTGGTCCATCGGACATCCAGATGACCCAGTCTCCATCC TCCCTGTCTGCATCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGT CGTCCGATTGGGACGATGTTAAGTTGGTACCAGCAGAAACCAGGGAAAGCC CCTAAGCTCCTGATCCTTGCTTTTTCCCGTTTGCAAAGTGGGGTCCCATCA CGTTTCAGTGGCAGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGT CTGCAACCTGAAGATTTTGCTACGTACTACTGCGCGCAGGCTGGGACGCAT CCTACGACGTTCGGCCAAGGGACCAAGGTGGAAATCAAACGG Nucleotide plus myc tag sequence (SEQ ID NO: 334) GAGGTGCAGCTGTTGGAGTCTGGGGGAGGCTTGGTACAGCCTGGGGGGTCC CTGCGTCTCTCCTGTGCAGCCTCCGGATTCACCTTTAATAGGTATAGTATG GGGTGGCTCCGCCAGGCTCCAGGGAAGGGTCTAGAGTGGGTCTCACGGATT GATTCTTATGGTCGTGGTACATACTACGAAGACCCCGTGAAGGGCCGGTTC AGCATCTCCCGCGACAATTCCAAGAACACGCTGTATCTGCAAATGAACAGC CTGCGTGCCGAGGACACCGCCGTATATTACTGTGCGAAAATTTCTCAGTTT GGGTCAAATGCGTTTGACTACTGGGGTCAGGGAACCCAGGTCACCGTCTCG AGCGCTAGCACCAGTGGTCCATCGGACATCCAGATGACCCAGTCTCCATCC TCCCTGTCTGCATCTGTAGGAGACCGTGTCACCATCACTTGCCGGGCAAGT CGTCCGATTGGGACGATGTTAAGTTGGTACCAGCAGAAACCAGGGAAAGCC CCTAAGCTCCTGATCCTTGCTTTTTCCCGTTTGCAAAGTGGGGTCCCATCA CGTTTCAGTGGCAGTGGATCTGGGACAGATTTCACTCTCACCATCAGCAGT CTGCAACCTGAAGATTTTGCTACGTACTACTGCGCGCAGGCTGGGACGCAT CCTACGACGTTCGGCCAAGGGACCAAGGTGGAAATCAAACGGGCGGCCGCA GAACAAAAACTCATCTCAGAAGAGGATCTGAATTAA Where a myc-tagged molecule is indicated in this table, this was the version used in PK studies in the examples. Where no myc-tagged sequences are given, the PK studies in the examples were not done with myc-tagged material, ie, the studies were done with the non-tagged constructs shown.

EXEMPLIFICATION

All numbering in the experimental section is according to Kabat (Kabat, E. A. National Institutes of Health (US) & Columbia University. Sequences of proteins of immunological interst, edn 5 (US Dept. Of Health and Human Services Public Health Service, National Institues of Health, Bethesda, Md., 1991)).

Derivation of DOM7h-11 and DOM7h-14 variants is described. DOM7h-14 variants are not according to the invention.

Example 1: Vk Affinity Maturation Selections:

HSA (Human Serum Albumin) and RSA (Rat Serum Albumin) antigens were obtained from Sigma (essentially fatty acid free, ˜99% (agarose gel electrophoresis), lyophilized powder Cat. No. A3782 and A6414 respectively)

Biotinylated products of above two antigens were made by using EZ Link Sulfo-NHS-SS-Biotin (Pierce, Cat. No. 21331). Free biotin reagent was removed by passing the samples twice through PD10 desalting column followed by overnight dialysis against 1000× excess volume of PBS at 4° C. Resulting product was tested by mass spec and 1-2 biotins per molecule were observed.

Affinity Maturation Libraries:

Both error-prone and CDR libraries were created using DOM7h-11 and DOM7h-14 parental dAbs (see WO2008/096158 for the sequences of DOM7h-11 and DOM7h-14). The CDR libraries were generated in the pDOM4 vector and the error prone libraries were generated in the pDOM33 vector (to allow for selection with or without protease treatment). Vector pDOM4, is a derivative of the Fd phage vector in which the gene III signal peptide sequence is replaced with the yeast glycolipid anchored surface protein (GAS) signal peptide. It also contains a c-myc tag between the leader sequence and gene III, which puts the gene III back in frame. This leader sequence functions well both in phage display vectors but also in other prokaryotic expression vectors and can be universally used. pDOM33 is a modified version of the pDOM4 vector where the c-myc tag has been removed which renders the dAb-phage fusion resistant to the protease trypsin. This allows the use of trypsin within the phage selection to select for dAbs that are more protease stable (see WO2008149143).

For error-prone maturation libraries, plasmid DNA encoding the dAb to be matured was amplified by PCR, using the GENEMORPH® II RANDOM MUTAGENESIS KIT (random, unique mutagenesis kit, Stratagene). The product was digested with Sal I and Not I and used in a ligation reaction with cut phage vector pDOM33.

For the CDR libraries, PCR reactions were performed using degenerate oligonucleotides containing NNK or NNS codons to diversify the required positions in the dAb to be affinity matured. Assembly PCR was then used to generate a full length diversified insert. The insert was digested with Sal I and Not I and used in a ligation reaction with pDOM4 for mutagenesis of multiple residues and pDOM5 for mutagenesis of single residues. The pDOM5 vector is a pUC119-based expression vector where protein expression is driven by the LacZ promoter. A GAS1 leader sequence (see WO 2005/093074) ensures secretion of isolated, soluble dAbs into the periplasm and culture supernatant of E. coli. dAbs are cloned SalI/NotI in this vector, which appends a myc tag at the C-terminus of the dAb. This protocol using SalI and Not I results in inclusion of an ST amino acid sequence at the N-terminus.

The ligation produced by either method was then used to transform E. coli strain TB1 by electroporation and the transformed cells plated on 2×TY agar containing 15 μg/ml tetracycline, yielding library sizes of >5×10⁷ clones.

The error-prone libraries had the following average mutation rate and size: DOM7h-11 (2.5 mutations per dAb), size: 6.1×10⁸, DOM7h-14 (2.9 mutations per dAb), size: 5.4×10⁸.

Each CDR library has four amino acid diversity. Two libraries were generated for each of CDRs 1 and 3, and one library for CDR2. The positions diversified within each library are as follows (amino acids based on VK dummy DPK9 sequence):

Library size DOM7h-11 DOM7h-14 1 - Q27, S28, S30, S31 (CDR1) 8.8 × 10⁷ 5.8 × 10⁷ 2 - S30, S31, Y32, N34 (CDR1) 4.6 × 10⁸ 4.2 × 10⁸ 3 - Y49, A50, A51, S53 (CDR2) 3.9 × 10⁸ 2.4 × 10⁸ 4 - Q89, S91, Y92, S93 (CDR3) 1.8 × 10⁸ 2.5 × 10⁸ 5 - Y92, Y93, T94, N96 (CDR3) 4.0 × 10⁸ 3.3 × 10⁸

Example 2: Selection Strategies

Three phage selection strategies were adopted for Vκ ALBUDAB™ (anti-serum albumin dAb) affinity maturation:

-   -   1) Selections against HSA only:     -   Three rounds of selection against HSA were carried out. The         error prone libraries and each CDR library were selected as an         individual pool in all rounds. The first round of selection was         performed against HSA passively coated onto an immunotube at 1         mg/ml. Round 2 was performed against 100 nM HSA and round 3         against 10 nM (CDR selections) or 20 or 100 nM (Error prone         selections) HSA, both as soluble selections followed by a fourth         round of selection with the error prone libraries against 1.5 nM         HSA as a soluble selection. The error prone libraries were         eluted with 0.1M glycine pH 2.0 before neutralisation with 1M         Tris pH 8.0 and the CDR libraries were eluted with 1 mg/ml         trypsin before infection into log phase TG1 cells. The third         round of each selection was subcloned into pDOM5 for screening.         Soluble selections used biotinylated HSA.     -   2) Trypsin selections against HSA:     -   In order to select dAbs with increased protease resistance         compared to the parental clone and with potentially improved         biophysical properties, trypsin was used in phage selections         (see WO2008149143). Four rounds of selection were preformed         against HSA. The first round of selection of error prone         libraries was performed against passively coated HSA at 1 mg/ml         without trypsin; the second round against passively coated HSA         at 1 mg/ml with 20 μg/ml trypsin for 1 hour at 37° C.; the third         round selection was performed by soluble selection using         biotinylated HSA against 100 nM HSA with 20 μg/ml or 100 μg/ml         trypsin for 1 hour at 37° C. The final round of selection was         performed by soluble selection using biotinylated HSA against         100 nM HSA with 100 μg/ml trypsin overnight at 37° C.     -   3) Cross-over selections against HSA (round 1) and RSA (rounds         2-4):     -   The first round selection was carried out against 1 mg/ml         passively coated HSA or 1

HSA (soluble selection), followed by a further three rounds of soluble selections against biotinylated RSA at concentrations of 1 μM for round 1, 100 nm for round 2 and 20 nM, 10 nM or 1 nM for round 3.

Screening Strategy and Affinity Determination:

In each case after selection a pool of phage DNA from the appropriate round of selection is prepared using a QIAfilter midiprep kit (Qiagen), the DNA is digested using the restriction enzymes Sal1 and Not1 and the enriched V genes are ligated into the corresponding sites in pDOM5 the soluble expression vector which expresses the dAb with a myc tag (see PCT/EP2008/067789). The ligated DNA is used to electro-transform E. coli HB 2151 cells which are then grown overnight on agar plates containing the antibiotic carbenicillin. The resulting colonies are individually assessed for antigen binding. In each case at least 96 clones were tested for binding to HSA, CSA (Cynomlgus monkey Serum Albumin), MSA (mouse serum albumin) and RSA by BIACORE™ (surface plasmon resonance). MSA antigen was obtained from Sigma (essentially fatty acid free, ˜99% (agarose gel electrophoresis), lyophilized powder Cat. No. A3559) and CSA was purified from Cynomolgus serum albumin using prometic blue resin (Amersham). Soluble dAb fragments were produced in bacterial culture in ONEX culture media (Novagen) overnight at 37° C. in 96 well plates. The culture supernatant containing soluble dAb was centrifuged and analysed by BiaCore™ for binding to high density HSA, CSA, MSA and RSA CM5 chips. Clones were found to bind to all these species of serum albumin by off-rate screening. The clones were sequenced revealing unique dAb sequences.

The minimum identity to parent (at the amino acid level) of the clones selected was 97.2% (DOM7h-11-3: 97.2%, DOM7h-11-12: 98.2%, DOM7h11-15: 96.3%, DOM7h-11-18: 98.2%, DOM7h-11-19: 97.2%)

The minimum identity to parent (at the amino acid level) of the clones selected was 96.3% (DOM7h-14-10: 96.3%, DOM7h-14-18: 96.3%, DOM7h-14-19: 98.2%, DOM7h-14-28: 99.1%, DOM7h-14-36: 97.2%)

Unique dAbs were expressed as bacterial supernatants in 2.5 L shake flasks in Onex media at 30° C. for 48 hrs at 250 rpm. dAbs were purified from the culture media by absorption to protein L agarose followed by elution with 10 mM glycine pH2.0. Binding to HSA, CSA, MSA and RSA by BiaCore™ was confirmed using purified protein at 3 concentrations 1 μM, 500 nM and 50 nM. To determine the binding affinity (K_(D)) of the ALBUDABs™ to each serum albumin; purified dAbs were analysed by BiaCore™ over albumin concentration range from 5000 nM to 39 nM (5000 nM, 2500 nM, 1250 nM, 625 nM, 312 nM, 156 nM, 78 nM, 39 nM).

TABLE 6 Affinity (K_(D)) ALBUDAB ™ to SA (nM) Kd Ka Rat DOM7h-14 60 2.095E−01 4.00E+06 DOM7h-14-10 4 9.640E−03 4.57E+06 DOM7h-14-18 410 2.275E−01 5.60E+05 DOM 7h-14-19 890 2.870E−01 3.20E+05 DOM 7h-14-28 45 (140) 7.0E−02 (1.141e−1) 2.10E+06 (8.3e5) DOM 7h-14-36 30 (6120) 2.9E−02 (5.54e−2) 1.55E+06 (9e3) DOM 7h-11 2100 1.00E−01 4.80E+04 DOM 7h-11-3 10000 (88000) (7.18e−1) (8.11e3) DOM 7h-11-12 200 5.22E−01 2.76E+06 DOM 7h-11-15 20 2.10E−02 1.10E+06 DOM 7h-11-18 80 (29000) 6.0E−02 (3.7e−1) 1.64E+06 (1.3e4) DOM 7h-11-19 28 (17000) 9.1e−02 (1.4e−1) 9.80E+05 (8.1e3) Cyno DOM 7h-14 66 9.65E−02 1.50E+06 DOM 7h-14-10 9 1.15E−02 1.60E+06 DOM 7h-14-18 180 1.05E−01 6.30E+5  DOM 7h-14-19 225 1.56E−01 7.00E+05 DOM 7h-14-28 66 (136) 1.3E−01 (1.34e−1) 2.50E+06 (9.8e5) DOM 7h-14-36 35 (7830) 1.9E−02 (1.1e−1) 9.80E+06 (1.43e4) DOM 7h-11 1000 6.82E−01 8.00E+05 DOM 7h-11-3 670 (200) 9.6E−02 (1.5e−1) 2.90E+05 (7.26e5) DOM 7h-11-12 >6000 DOM 7h-11-15 3 5.57E−03 5.80E+06 DOM 7h-11-18 10000 (65000) 1.36 (4.8e−1) 2.25E+05 (7.3e3) DOM 7h-11-19 >10000 (375000) (6.2e−1) (1.7e3) Mouse DOM 7h-14 12 4.82E−02 4.10E+06 DOM 7h-14-10 30 3.41E−02 1.29E+06 DOM 7h-14-18 65 9.24E−02 2.28E+06 DOM 7h-14-19 60 5.76E−02 1.16E+06 DOM 7h-14-28 26 (31) 3.4E−02 (7.15e−2) 1.60E+06 (2.28e6) DOM 7h-14-36 35 (33) 2.3E−02 (7.06e−2) 8.70E+05 (2.11e6) DOM 7h-11 5000 9.00E−01 DOM 7h-11-3 >10000 (36000) (6.12e−1) (1.67e4) DOM 7h-11-12 130 1.89E−01 1.53E+06 DOM 7h-11-15 10 9.40E−03 1.10E+06 DOM 7h-11-18 150 (1600) 2.4E−02 (6.23e−2) 4.40E+05 (4e4) DOM 7h-11-19 100 (18000) 3.7E−02 (8.8e−2) 1.40E+06 (4.9e3) Human DOM 7h-14 33 4.17E−02 1.43E+06 DOM 7h-14-10 12 1.39E−02 1.50E+06 DOM 7h-14-18 280 3.39E−02 1.89E+05 DOM 7h-14-19 70 5.25E−02 8.26E+05 DOM 7h-14-28 30 (8260) 3.3E−02 (5.6e−2) 1.24E+06 (6.78e3) DOM 7h-14-36 28 (1260) 2.4E−02 (6.7e−2) 1.23E+06 (5.4e4) DOM 7h-11 2800 6.41E−01 7.00E+05 DOM 7h-11-3 32 (130) 1.6E−02 (2.35e−2) 6.50E+05 (1.86e5) DOM 7h-11-12 350 4.13E−01 1.26E+06 DOM 7h-11-15 1 1.84E−03 2.00E+06 DOM 7h-11-18 36 (32000) 5.1E−02 (2.7e−1) 3.40E+06 (8.39e3) DOM 7h-11-19 65 (38000) 1.1E−01 (2.09e−1) 1.80E+06 (5.4e3) *: values in brackets were derived from a second, independent SPR experiment.

All DOM7h-14 derived variants are cross-reactive to mouse, rat, human and cyno serum albumin. DOM7h-14-10 has improved affinity to rat, cyno and human serum albumin compared to parent. DOM7h-14-28 has an improved affinity to RSA. DOM7h-14-36 has an improved affinity to RSA, CSA and MSA.

DOM7h-11-3 has improved affinity to CSA and HSA. DOM7h-11-12 has improved affinity to RSA, MSA and HSA. DOM7h-11-15 has improved affinity to RSA, MSA, CSA and HSA. DOM7h-11-18 and DOM7h-11-19 have improved affinity to RSA, MSA and HSA.

Example 3: Origins of Key DOM7h-11 Lineage Clones

DOM7h-11-3: From affinity maturation performed against HSA using the CDR2 library (Y49, A50, A51, S53), round 3 output 10 nM HSA

DOM7h-11-12: From affinity maturation performed against HSA using the error prone library, round 3 outputs (100 nM, HSA) with 100 ug/ml trypsin.

DOM7h-11-15: From cross-over selections performed against HSA as round 1 followed by additional 3 rounds of selections against RSA using the CDR2 library (Y49, A50, A51, S53) at round 3 selection with 1 nM of RSA.

DOM7h-11-18 From cross-over selections performed against HSA as round 1 followed by additional 3 rounds of selections against RSA using the error prone library, round 3 output at 20 nM of RSA

DOM7h-11-19 From cross-over selections performed against HSA as round 1 followed by additional 3 rounds of selections against RSA using the error prone library, round 3 output at 5 nM of RSA

TABLE 7 CDR sequences (according to Kabat;  ref. as above) CDR ALBUDAB ™ CDR1 CDR2 CDR3 DPK9 Vk SQSISSYLN YAASSLQS QQSYSTPNT dummy (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 335) 336) 337) DOM7h-11 SRPIGTTLS WFGSRLQS AQAGTHPTT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 338) 339) 340) DOM7h-11-12 SRPIGTMLS LFGSRLQS AQAGTHPTT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 341) 342) 343) DOM 7h-11-15 SRPIGTMLS LAFSRLQS AQAGTHPTT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 344) 345) 346) DOM 7h-11-18 SRPIGTMLS WFGSRLQS AQAGTHPTT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 347) 348) 349) DOM 7h-11-19 SRPIGTMLS LFGSRLQS AQTGTHPTT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 350) 351) 352) DOM 7h-11-3 SRPIGTTLS LWFSRLQS AQAGTHPTT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 353) 354) 355)

Example 4: Origins of Key DOM7h-14 Lineage Clones

DOM7h-14-19: From affinity maturation performed against HSA using the error prone library, round 3 outputs (100 nM, HSA) with 100 ug/ml trypsin.

DOM7h-14-10, DOM7h-14-18, DOM7h-14-28, DOM7h-14-36: From affinity maturation performed against HSA using CDR3 library (Y92, Y93, T94, N96), round 3 output.

TABLE 8 CDR sequences (according to Kabat; ref. as above) CDR ALBUDAB ™ CDR1 CDR2 CDR3 DPK9 Vk SQSISSYLN YAASSLQS QQSYSTPNT dummy (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 335) 336) 337) DOM 7h-14 SQWIGSQLS MWRSSLQS AQGAALPRT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 356) 357) 358) DOM 7h-14-10 SQWIGSQLS MWRSSLQS AQGLRHPKT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 359) 360) 361) DOM 7h-14-18 SQWIGSQLS MWRSSLQS AQGLMKPMT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 362) 363) 364) DOM 7h-14-19 SQWIGSQLS MWRSSLQS AQGAALPRT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 365) 366) 367) DOM 7h-14-28 SQWIGSQLS MWRSSLQS AQGAALPKT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 368) 369) 370) DOM 7h-14-36 SQWIGSQLS MWRSSLQS AQGFKKPRT (SEQ ID NO: (SEQ ID NO: (SEQ ID NO: 371) 372) 373)

Example 5: Expression and Biophysical Characterisation

The routine bacterial expression level in 2.5 L shake flasks was determined following culture in Onex media at 30° C. for 48 hrs at 250 rpm. The biophysical characteristics were determined by SEC MALLS and DSC.

SEC MALLS (size exclusion chromatography with multi-angle-LASER-light-scattering) is a non-invasive technique for the characterizing of macromolecules in solution. Briefly, proteins (at concentration of 1 mg/mL in buffer Dulbecco's PBS at 0.5 ml/min are separated according to their hydrodynamic properties by size exclusion chromatography (column: TSK3000 from TOSOH Biosciences; 5200 from Pharmacia). Following separation, the propensity of the protein to scatter light is measured using a multi-angle-LASER-light-scattering (MALLS) detector. The intensity of the scattered light while protein passes through the detector is measured as a function of angle. This measurement taken together with the protein concentration determined using the refractive index (RI) detector allows calculation of the molar mass using appropriate equations (integral part of the analysis software Astra v.5.3.4.12).

DSC (Differential Scanning calorimetry): briefly, the protein is heated at a constant rate of 180° C./hrs (at 1 mg/mL in PBS) and a detectable heat change associated with thermal denaturation measured. The transition midpoint (_(app)T_(m)) is determined, which is described as the temperature where 50% of the protein is in its native conformation and the other 50% is denatured. Here, DSC determined the apparent transition midpoint (appTm) as most of the proteins examined do not fully refold. The higher the Tm, the more stable the molecule. Unfolding curves were analysed by non-2-state equations. The software package used was Origin^(R) v7.0383.

TABLE 9 Biophysical parameters ALBUDAB ™ SEC MALLS DSC Tm(° C.) DOM7h-14 M 60 DOM 7h-14-10 M 59 DOM 7h-14-18 M 58 DOM 7h-14-19 M 59 DOM 7h-14-28 M 58.3/60.2 DOM 7h-14-36 M   59.2 DOM 7h-11 M 66.9-72.2 DOM 7h-11-3 M (95%)* 66.6/70.5 DOM 7h-11-12 M (<2% D)   71.7 DOM 7h-11-15 M (<5% D) 58.5-60.5 DOM 7h-11-18 M (98%) 58.9/65.8 DOM 7h-11-19 M 71.8/76.6 *in one other trial, monomer was primarily seen by SEC MALLS, although lower than 95% We observed expression levels for all clones in Table 9 in the range from 15 to 119 mg/L in E coli.

For DOM7h-14 and DOM7h-11 variants, favorable biophysical parameters (monomeric in solution as determined by SEC MALLs and appTm of >55° C. as determined by DSC) and expression levels were maintained during affinity maturation. Monomeric state is advantageous because it avoids dimerisation and the risk of products that may cross-link targets such as cell-surface receptors.

Example 6: Determination of Serum Half Life in Rat, Mouse and Cynomolgus Monkey

ALBUDABs™ DOM7h-14-10, DOM7h-14-18, DOM7h-14-19, DOM7h-11, DOM7h11-12 and DOM7h-11-15 were cloned into the pDOM5 vector. For each ALBUDAB™, 20-50 mg quantities were expressed in E. coli and purified from bacterial culture supernatant using protein L affinity resin and eluted with 100 mM glycine pH2. The proteins were concentred to greater than 1 mg/ml, buffer exchanged into PBS and endotoxin depleted using Q spin columns (Vivascience). For Rat pharmacokinetic (PK) analysis, ALBUDABs™ were dosed as single i.v injections at 2.5 mg/kg using 3 rats per compound. Serum samples were taken at 0.16, 1, 4, 12, 24, 48, 72, 120, 168 hrs. Analysis of serum levels was by anti-myc ELISA as per the method described below.

For Mouse PK, DOM7h-11, DOM7h11-12 and DOM7h-11-15 were dosed as single i.v injections at 2.5 mg/kg per dose group of 3 subjects and serum samples taken at 10 mins; 1 h; 8 h; 24 h; 48 h; 72 h; 96 h. Analysis of serum levels was by anti-myc ELISA as per the method described below.

For Cynomolgus monkey PK DOM7h-14-10 and DOM7h-11-15 were dosed as single i.v injections at 2.5 mg/kg into 3 female Cynomolgus monkeys per dose group and serum samples taken at 0.083, 0.25, 0.5, 1, 2, 4, 8, 24, 48, 96, 144, 192, 288, 336, 504 hrs. Analysis of serum levels was by anti-myc ELISA as per the method described below.

Anti-Myc ELISA Method

The ALBUDAB™ concentration in serum was measured by anti-myc ELISA. Briefly, goat anti-myc polyclonal antibody (1:500; Abcam, catalogue number ab9132) was coated overnight onto Nunc 96-well Maxisorp plates and blocked with 5% BSA/PBS+1% tween. Serum samples were added at a range of dilutions alongside a standard at known concentrations. Bound myc-tagged ALBUDAB′ was then detected using a rabbit polyclonal anti-Vk (1:1000; in-house reagent, bleeds were pooled and protein A purified before use) followed by an anti-rabbit IgG HRP antibody (1:10,000; Sigma, catalogue number A2074). Plates were washed between each stage of the assay with 3×PBS+0.1% Tween20 followed by 3×PBS. TMB (SureBlue TMB 1-Component Microwell Peroxidase Substrate, KPL, catalogue number 52-00-00) was added after the last wash and was allowed to develop. This was stopped with 1M HCl and the signal was then measured using absorbance at 450 nm.

From the raw ELISA data, the concentration of unknown samples was established by interpolation against the standard curve taking into account dilution factors. The mean concentration result from each time point was determined from replicate values and entered into WinNonLin analysis package (eg version 5.1 (available from Pharsight Corp., Mountain View, Calif. 94040, USA). The data was fitted using a non-compartmental model, where PK parameters were estimated by the software to give terminal half-lives. Dosing information and time points were selected to reflect the terminal phase of each PK profile.

TABLE 10 Single ALBUDAB ™ PK PK parameters Albumin AUC CL t½ Vz Species ALBUDAB ™ K_(D) (nM) h × μg/ml ml/h/kg h ml/kg Rat DOM7h-14* 60 DOM7h-14-10 4 2134.6 1.2 42.1 71.2 DOM7h-14-18 410 617.3 4.1 38.4 228.1 DOM 7h-14-19 890 632.6 4.1 36.3 213.3 DOM 7h-11 2100 320.1 7.8 23.3 263.9 DOM 7h-11-12 200 398.7 6.4 35.5 321.2 DOM 7h-11-15 20 843.4 3.0 30.3 130.7 mouse DOM 7h-11 5000 304.7 8.2 18.3 216.8 DOM 7h-11-12 130 646.6 3.9 43.9 244.8 DOM 7h-11-15 10 499.2 5.0 33.7 243.4 Cyno DOM 7h-14* 66 217.5 DOM 7h-14-10 9 6174.6 0.4 200.8 117.8 DOM 711-11* 3300 135.1 DOM 7h-11-15 3 4195 0.6 198.1 170.3 *Historical data

Pharmacokinetic parameters derived from rat, mouse and cynomolgus monkey studies were fitted using a non-compartmental model. Key: AUC: Area under the curve from dosing time extrapolated to infinity; CL: clearance; t½: is the time during which the blood concentration is halved; Vz: volume of distribution based on the terminal phase.

DOM7h-11 12 and DOM7h-11-15 have an improved AUC and t1/2 in rat and mouse compared to parent. DOM7h-11-15 also has an improved AUC and t1/2 in cyno compared to parent. This improvement in AUC/t1/2 correlates with an improved in vitro KD to serum albumin.

Example 7: ALBUDAB™ IFN Fusions Cloning and Expression

As well as single ALBUDABs™, the affinity matured Vk ALBUDABs™ were linked to Interferon alpha 2b (IFNα2b) to determine whether a useful PK of the ALBUDAB™ was maintained as a fusion protein.

Interferon alpha 2b amino acid sequence: (SEQ ID NO: 374) CDLPQTHSLGSRRTLMLLAQMRRISLFSCLKDRHDFGFPQEEFGNQFQKA ETIPVLHEMIQQIFNLFSTKDSSAAWDETLLDKFYTELYQQLNDLEACVI QGVGVTETPLMKEDSILAVRKYFQRITLYLKEKKYSPCAWEVVRAEIMRS FSLSTNLQESLRSKE Interferon alpha 2b nucleotide sequence: (SEQ ID NO: 375) TGTGATCTGCCTCAAACCCACAGCCTGGGTAGCAGGAGGACCTTGATGCT CCTGGCACAGATGAGGAGAATCTCTCTTTTCTCCTGCTTGAAGGACAGAC ATGACTTTGGATTTCCCCAGGAGGAGTTTGGCAACCAGTTCCAAAAGGCT GAAACCATCCCTGTCCTCCATGAGATGATCCAGCAGATCTTCAATCTCTT CAGCACAAAGGACTCATCTGCTGCTTGGGATGAGACCCTCCTAGACAAAT TCTACACTGAACTCTACCAGCAGCTGAATGACCTGGAAGCCTGTGTGATA CAGGGGGTGGGGGTGACAGAGACTCCCCTGATGAAGGAGGACTCCATTCT GGCTGTGAGGAAATACTTCCAAAGAATCACTCTCTATCTGAAAGAGAAGA AATACAGCCCTTGTGCCTGGGAGGTTGTCAGAGCAGAAATCATGAGATCT TTTTCTTTGTCAACAAACTTGCAAGAAAGTTTAAGAAGTAAGGAA

IFNa2b was linked to the ALBUDAB™ via a TVAAPS (SEQ ID NO: 422) linker region (see WO2007085814). The constructs were cloned by SOE-PCR (single overlap extension according to the method of Horton et al. Gene, 77, p 61 (1989)). PCR amplification of the ALBUDAB™ and IFN sequences were carried out separately using primers with a ˜15 base pair overlap at the TVAAPS (SEQ ID NO: 422) linker region. The primers used are as follows:—

IFNα2b SOE fragment 5′ (SEQ ID NO: 376) GCCCGGATCCACCGGCTGTGATCTG IFNα2b SOE fragment 3′ (SEQ ID NO: 377) GGAGGATGGAGACTGGGTCATCTGGATGTC Vk SOE fragment 5′ (SEQ ID NO: 378) GACATCCAGATGACCCAGTCTCCATCCTCC Vk SOE fragment 3′ to also introduce a myc tag (SEQ ID NO: 379) GCGCAAGCTTTTATTAATTCAGATCCTCTTC TGAGATGAGTTTTTGTTCTGCGGCCGCCCGT TTGATTTCCACCTTGGTCCC

The fragments were purified separately and subsequently assembled in a SOE (single overlap extension PCR extension) reaction using only the flanking primers.

IFNα2b SOE fragment 5′ (SEQ ID NO: 380) GCCCGGATCCACCGGCTGTGATCTG Vk SOE fragment 3′ to also introduce a myc tag (SEQ ID NO: 381) GCGCAAGCTTTTATTAATTCAGATCCTCTTC TGAGATGAGTTTTTGTTCTGCGGCCGCCCGT TTGATTTCCACCTTGGTCCC

The assembled PCR product was digested using the restriction enzymes BamHI and HindIII and the gene ligated into the corresponding sites in the pDOM50, a mammalian expression vector which is a pTT5 derivative with an N-terminal V-J2-C mouse IgG secretory leader sequence to facilitate expression into the cell media.

Leader sequence (amino acid): (SEQ ID NO: 382) METDTLLLWVLLLWVPGSTG Leader sequence (nucleotide): (SEQ ID NO: 383) ATGGAGACCGACACCCTGCTGCTGTGGGTGCTGCTGCTGTGGGTGCCCGG ATCCACCGGGC

Plasmid DNA was prepared using QIAfilter megaprep (Qiagen). 1 μg DNA/ml was transfected with 293-Fectin into HEK293E cells and grown in serum free media. The protein is expressed in culture for 5 days and purified from culture supernatant using protein L affinity resin and eluted with 100 mM glycine pH2. The proteins were concentred to greater than 1 mg/ml, buffer exchanged into PBS and endotoxin depleted using Q spin columns (Vivascience).

TABLE 11 Interferon alpha 2b-ALBUDAB ™ sequences with and without myc-tag (as amino acid- and nucleotide sequence) The Interferon alpha 2b is N-terminal to the ALBUDAB ™ in the following fusions. aa + myc nt + myc aa no tag nt no tag DMS7321 CDLPQTHSLGSRRT TGCGACTTGCC CDLPQTHSLG TGCGACTTGCC (IFNα2b- LMLLAQMRRISLFS ACAGACACAT SRRTLMLLA ACAGACACAT DOM7h- CLKDRHDFGFPQE AGTTTGGGATC QMRRISLFSC AGTTTGGGATC 14) EFGNQFQKAETIPV AAGAAGAACA LKDRHDFGFP AAGAAGAACA LHEMIQQIFNLFST TTGATGTTATT QEEFGNQFQ TTGATGTTATT KDSSAAWDETLLD AGCACAAATG KAETIPVLHE AGCACAAATG KFYTELYQQLNDL CGTAGAATTTC MIQQIFNLFS CGTAGAATTTC EACVIQGVGVTETP TTTGTTCTCTT TKDSSAAWD TTTGTTCTCTT LMKEDSILAVRKY GTCTAAAGGAC ETLLDKFYTE GTCTAAAGGA FQRITLYLKEKKYS CGTCACGACTT LYQQLNDLE CCGTCACGACT PCAWEVVRAEIMR CGGATTCCCTC ACVIQGVGV TCGGATTCCCT SFSLSTNLQESLRS AGGAAGAGTTT TETPLMKEDS CAGGAAGAGT KETVAAPSDIQMT GGAAACCAATT ILAVRKYFQR TTGGAAACCA QSPSSLSASVGDRV CCAAAAAGCA ITLYLKEKKY ATTCCAAAAA TITCRASQWIGSQL GAAACTATTCC SPCAWEVVR GCAGAAACTA SWYQQKPGKAPKL TGTCTTGCACG AEIMRSFSLS TTCCTGTCTTG LIMWRSSLQSGVPS AAATGATCCAG TNLQESLRSK CACGAAATGA RFSGSGSGTDFTLT CAAATATTCAA ETVAAPSDIQ TCCAGCAAATA ISSLQPEDFATYYC TTTGTTTTCTA MTQSPSSLSA TTCAATTTGTT AQGAALPRTFGQG CAAAGGACTC SVGDRVTITC TTCTACAAAGG TKVEIKR ATCAGCCGCTT RASQWIGSQL  ACTCATCAGCC AAAEQKLISEEDL GGGATGAAAC SWYQQKPGK GCTTGGGATGA N* (SEQ ID NO: 384) TCTGTTAGATA APKLLIMWR AACTCTGTTAG AATTCTACACT SSLQSGVPSR ATAAATTCTAC GAACTATATCA FSGSGSGTDF ACTGAACTATA ACAACTGAAC TLTISSLQPED TCAACAACTGA GATCTAGAGGC FATYYCAQG ACGATCTAGA TTGCGTTATTC AALPRTFGQ GGCTTGCGTTA AGGGTGTAGG GTKVEIKR TTCAGGGTGTA AGTTACTGAAA (SEQ ID GGAGTTACTGA CTCCCCTAATG NO: 386) AACTCCCCTAA AAAGAAGATT TGAAAGAAGA CAATTCTAGCC TTCAATTCTAG GTTAGAAAATA CCGTTAGAAA CTTTCAGCGTA ATACTTTCAGC TCACATTGTAT GTATCACATTG TTAAAGGAAA TATTTAAAGGA AGAAATACTCC AAAGAAATAC CCATGTGCATG TCCCCATGTGC GGAGGTGGTTA ATGGGAGGTG GAGCAGAAAT GTTAGAGCAG TATGAGGTCCT AAATTATGAG TCTCTCTTTCT GTCCTTCTCTC ACGAATTTGCA TTTCTACGAAT AGAATCTTTGA TTGCAAGAATC GATCTAAGGA TTTGAGATCTA AACCGTCGCTG AGGAAACCGT CTCCATCTGAC CGCTGCTCCAT ATCCAGATGAC CTGACATCCAG CCAGTCTCCAT ATGACCCAGTC CCTCCCTGTCT TCCATCCTCCC GCATCTGTAGG TGTCTGCATCT AGACCGTGTCA GTAGGAGACC CCATCACTTGC GTGTCACCATC CGGGCAAGTC ACTTGCCGGGC AGTGGATTGGG AAGTCAGTGG TCTCAGTTATC ATTGGGTCTCA TTGGTACCAGC GTTATCTTGGT AGAAACCAGG ACCAGCAGAA GAAAGCCCCTA ACCAGGGAAA AGCTCCTGATC GCCCCTAAGCT ATGTGGCGTTC CCTGATCATGT CTCGTTGCAAA GGCGTTCCTCG GTGGGGTCCCA TTGCAAAGTGG TCACGTTTCAG GGTCCCATCAC TGGCAGTGGAT GTTTCAGTGGC CTGGGACAGAT AGTGGATCTGG TTCACTCTCAC GACAGATTTCA CATCAGCAGTC CTCTCACCATC TGCAACCTGAA AGCAGTCTGCA GATTTTGCTAC ACCTGAAGATT GTACTACTGTG TTGCTACGTAC CTCAGGGTGCG TACTGTGCTCA GCGTTGCCTAG GGGTGCGGCG GACGTTCGGCC TTGCCTAGGAC AAGGGACCAA GTTCGGCCAAG GGTGGAAATC GGACCAAGGT AAACGGGCGG GGAAATCAAA CCGCAGAACA CGG (SEQ ID AAAACTCATC NO: 387) TCAGAAGAGG ATCTGAATTA A (SEQ ID NO: 385) DMS732 CDLPQTHSLGSRRT TGCGACTTGCC CDLPQTHSLG TGCGACTTGCC (IFNα2b- LMLLAQMRRISLF SACAGACACAT SRRTLMLLA ACAGACACAT DOM7h- CLKDRHDFGFPQE AGTTTGGGATC QMRRISLFSC AGTTTGGGATC 14-10) EFGNQFQKAETIPV AAGAAGAACA LKDRHDFGFP AAGAAGAACA LHEMIQQIFNLFST TTGATGTTATT QEEFGNQFQ TTGATGTTATT KDSSAAWDETLLD AGCACAAATG KAETIPVLHE AGCACAAATG KFYTELYQQLNDL CGTAGAATTTC MIQQIFNLFS CGTAGAATTTC EACVIQGVGVTETP TTTGTTCTCTT TKDSSAAWD TTTGTTCTCTT LMKEDSILAVRKY GTCTAAAGGAC ETLLDKFYTE GTCTAAAGGA FQRITLYLKEKKYS CGTCACGACTT LYQQLNDLE CCGTCACGACT PCAWEVVRAEIMR CGGATTCCCTC ACVIQGVGV TCGGATTCCCT SFSLSTNLQESLRS AGGAAGAGTTT TETPLMKEDS CAGGAAGAGT KETVAAPSDIQMT GGAAACCAATT ILAVRKYFQR TTGGAAACCA QSPSSLSASVGDRV CCAAAAAGCA ITLYLKEKKY ATTCCAAAAA TITCRASQWIGSQL GAAACTATTCC SPCAWEVVR GCAGAAACTA SWYQQKPGKAPKL TGTCTTGCACG AEIMRSFSLS TTCCTGTCTTG LIMWRSSLQSGVPS AAATGATCCAG TNLQESLRSK CACGAAATGA RFSGSGSGTDFTLT CAAATATTCAA ETVAAPSDIQ TCCAGCAAATA ISSLQPEDFATYYC TTTGTTTTCTA MTQSPSSLSA TTCAATTTGTT AQGLRHPKTFGQG CAAAGGACTC SVGDRVTITC TTCTACAAAGG TKVEIKR ATCAGCCGCTT RASQWIGSQL ACTCATCAGCC AAAEQKLISEEDL GGGATGAAAC SWYQQKPGK GCTTGGGATGA N* (SEQ ID NO: 388) TCTGTTAGATA APKLLIMWR AACTCTGTTAG AATTCTACACT SSLQSGVPSR ATAAATTCTAC GAACTATATCA FSGSGSGTDF ACTGAACTATA ACAACTGAAC TLTISSLQPED TCAACAACTGA GATCTAGAGGC FATYYCAQG ACGATCTAGA TTGCGTTATTC LRHPKTFGQ GGCTTGCGTTA AGGGTGTAGG GTKVEIKR TTCAGGGTGTA AGTTACTGAAA (SEQ ID GGAGTTACTGA CTCCCCTAATG NO: 390) AACTCCCCTAA AAAGAAGATT TGAAAGAAGA CAATTCTAGCC TTCAATTCTAG GTTAGAAAATA CCGTTAGAAA CTTTCAGCGTA ATACTTTCAGC TCACATTGTAT GTATCACATTG TTAAAGGAAA TATTTAAAGGA AGAAATACTCC AAAGAAATAC CCATGTGCATG TCCCCATGTGC GGAGGTGGTTA ATGGGAGGTG GAGCAGAAAT GTTAGAGCAG TATGAGGTCCT AAATTATGAG TCTCTCTTTCT GTCCTTCTCTC ACGAATTTGCA TTTCTACGAAT AGAATCTTTGA TTGCAAGAATC GATCTAAGGA TTTGAGATCTA AACCGTCGCTG AGGAAACCGT CTCCATCTGAC CGCTGCTCCAT ATCCAGATGAC CTGACATCCAG CCAGTCTCCAT ATGACCCAGTC CCTCCCTGTCT TCCATCCTCCC GCATCTGTAGG TGTCTGCATCT AGACCGTGTCA GTAGGAGACC CCATCACTTGC GTGTCACCATC CGGGCAAGTC ACTTGCCGGGC AGTGGATTGGG AAGTCAGTGG TCTCAGTTATC ATTGGGTCTCA TTGGTACCAGC GTTATCTTGGT AGAAACCAGG ACCAGCAGAA GAAAGCCCCTA ACCAGGGAAA AGCTCCTGATC GCCCCTAAGCT ATGTGGCGTTC CCTGATCATGT CTCGTTGCAAA GGCGTTCCTCG GTGGGGTCCCA TTGCAAAGTGG TCACGTTTCAG GGTCCCATCAC TGGCAGTGGAT GTTTCAGTGGC CTGGGACAGAT AGTGGATCTGG TTCACTCTCAC GACAGATTTCA CATCAGCAGTC CTCTCACCATC TGCAACCTGAA AGCAGTCTGCA GATTTTGCTAC ACCTGAAGATT GTACTACTGTG TTGCTACGTAC CTCAGGGTTTG TACTGTGCTCA AGGCATCCTAA GGGTTTGAGGC GACGTTCGGCC ATCCTAAGACG AAGGGACCAA TTCGGCCAAGG GGTGGAAATC GACCAAGGTG AAACGGGCGG GAAATCAAAC CCGCAGAACA GG (SEQ ID AAAACTCATC NO: 391) TCAGAAGAGG ATCTGAATTA A (SEQ ID NO: 389) DMS7323 CDLPQTHSLGSRRT TGCGACTTGCC CDLPQTHSLG TGCGACTTGCC (IFNα2b- LMLLAQMRRISLF SACAGACACAT SRRTLMLLA ACAGACACAT DOM7h- CLKDRHDFGFPQE AGTTTGGGATC QMRRISLFSC AGTTTGGGATC 14-18) EFGNQFQKAETIPV AAGAAGAACA LKDRHDFGFP AAGAAGAACA LHEMIQQIFNLFST TTGATGTTATT QEEFGNQFQ TTGATGTTATT KDSSAAWDETLLD AGCACAAATG KAETIPVLHE AGCACAAATG KFYTELYQQLNDL CGTAGAATTTC MIQQIFNLFS CGTAGAATTTC EACVIQGVGVTETP TTTGTTCTCTT TKDSSAAWD TTTGTTCTCTT LMKEDSILAVRKY GTCTAAAGGAC ETLLDKFYTE GTCTAAAGGA FQRITLYLKEKKYS CGTCACGACTT LYQQLNDLE CCGTCACGACT PCAWEVVRAEIMR CGGATTCCCTC ACVIQGVGV TCGGATTCCCT SFSLSTNLQESLRS AGGAAGAGTTT TETPLMKEDS CAGGAAGAGT KETVAAPSDIQMT GGAAACCAATT ILAVRKYFQR TTGGAAACCA QSPSSLSASVGDRV CCAAAAAGCA ITLYLKEKKY ATTCCAAAAA TITCRASQWIGSQL GAAACTATTCC SPCAWEVVR GCAGAAACTA SWYQQKPGKAPKL TGTCTTGCACG AEIMRSFSLS TTCCTGTCTTG LIMWRSSLQSGVPS AAATGATCCAG TNLQESLRSK CACGAAATGA RFSGSGSGTDFTLT CAAATATTCAA ETVAAPSDIQ TCCAGCAAATA ISSLQPEDFATYYC TTTGTTTTCTA MTQSPSSLSA TTCAATTTGTT AQGLMKPMTFGQ CAAAGGACTC SVGDRVTITC TTCTACAAAGG GTKVEIKRAAAEQ ATCAGCCGCTT RASQWIGSQL ACTCATCAGCC KLISEEDLN* (SEQ GGGATGAAAC SWYQQKPGK GCTTGGGATGA ID NO: 392) TCTGTTAGATA APKLLIMWR AACTCTGTTAG AATTCTACACT SSLQSGVPSR ATAAATTCTAC GAACTATATCA FSGSGSGTDF ACTGAACTATA ACAACTGAAC TLTISSLQPED TCAACAACTGA GATCTAGAGGC FATYYCAQG ACGATCTAGA TTGCGTTATTC LMKPMTFGQ GGCTTGCGTTA AGGGTGTAGG GTKVEIKR TTCAGGGTGTA AGTTACTGAAA (SEQ ID GGAGTTACTGA CTCCCCTAATG NO: 394) AACTCCCCTAA AAAGAAGATT TGAAAGAAGA CAATTCTAGCC TTCAATTCTAG GTTAGAAAATA CCGTTAGAAA CTTTCAGCGTA ATACTTTCAGC TCACATTGTAT GTATCACATTG TTAAAGGAAA TATTTAAAGGA AGAAATACTCC AAAGAAATAC CCATGTGCATG TCCCCATGTGC GGAGGTGGTTA ATGGGAGGTG GAGCAGAAAT GTTAGAGCAG TATGAGGTCCT AAATTATGAG TCTCTCTTTCT GTCCTTCTCTC ACGAATTTGCA TTTCTACGAAT AGAATCTTTGA TTGCAAGAATC GATCTAAGGA TTTGAGATCTA AACCGTCGCTG AGGAAACCGT CTCCATCTGAC CGCTGCTCCAT ATCCAGATGAC CTGACATCCAG CCAGTCTCCAT ATGACCCAGTC CCTCCCTGTCT TCCATCCTCCC GCATCTGTAGG TGTCTGCATCT AGACCGTGTCA GTAGGAGACC CCATCACTTGC GTGTCACCATC CGGGCAAGTC ACTTGCCGGGC AGTGGATTGGG AAGTCAGTGG TCTCAGTTATC ATTGGGTCTCA TTGGTACCAGC GTTATCTTGGT AGAAACCAGG ACCAGCAGAA GAAAGCCCCTA ACCAGGGAAA AGCTCCTGATC GCCCCTAAGCT ATGTGGCGTTC CCTGATCATGT CTCGTTGCAAA GGCGTTCCTCG GTGGGGTCCCA TTGCAAAGTGG TCACGTTTCAG GGTCCCATCAC TGGCAGTGGAT GTTTCAGTGGC CTGGGACAGAT AGTGGATCTGG TTCACTCTCAC GACAGATTTCA CATCAGCAGTC CTCTCACCATC TGCAACCTGAA AGCAGTCTGCA GATTTTGCTAC ACCTGAAGATT GTACTACTGTG TTGCTACGTAC CTCAGGGTCTT TACTGTGCTCA ATGAAGCCTAT GGGTCTTATGA GACGTTCGGCC AGCCTATGACG AAGGGACCAA TTCGGCCAAGG GGTGGAAATC GACCAAGGTG AAACGGGCGG GAAATCAAAC CCGCAGAACA GG (SEQ ID AAAACTCATC NO: 395) TCAGAAGAGG ATCTGAATTA A (SEQ ID NO: 393) DMS7324 CDLPQTHSLGSRRT TGCGACTTGCC CDLPQTHSLG TGCGACTTGCC (IFNα2b- LMLLAQMRRISLF SACAGACACAT SRRTLMLLA ACAGACACAT DOM7h- CLKDRHDFGFPQE AGTTTGGGATC QMRRISLFSC AGTTTGGGATC 14-19) EFGNQFQKAETIPV AAGAAGAACA LKDRHDFGFP AAGAAGAACA LHEMIQQIFNLF STTTGATGTTATT QEEFGNQFQ TTGATGTTATT KDSSAAWDETLLD AGCACAAATG KAETIPVLHE AGCACAAATG KFYTELYQQLNDL CGTAGAATTTC MIQQIFNLFS CGTAGAATTTC EACVIQGVGVTETP TTTGTTCTCTT TKDSSAAWD TTTGTTCTCTT LMKEDSILAVRKY GTCTAAAGGAC ETLLDKFYTE GTCTAAAGGA FQRITLYLKEKKYS CGTCACGACTT LYQQLNDLE CCGTCACGACT PCAWEVVRAEIMR CGGATTCCCTC ACVIQGVGV TCGGATTCCCT SFSLSTNLQESLRS AGGAAGAGTTT TETPLMKEDS CAGGAAGAGT KETVAAPSDIQMT GGAAACCAATT ILAVRKYFQR TTGGAAACCA QSPSSLSASVGDRV CCAAAAAGCA ITLYLKEKKY ATTCCAAAAA TISCRASQWIGSQL GAAACTATTCC SPCAWEVVR GCAGAAACTA SWYQQKPGEAPKL TGTCTTGCACG AEIMRSFSLS TTCCTGTCTTG LIMWRSSLQSGVPS AAATGATCCAG TNLQESLRSK CACGAAATGA RFSGSGSGTDFTLT CAAATATTCAA ETVAAPSDIQ TCCAGCAAATA ISSLQPEDFATYYC TTTGTTTTCTA MTQSPSSLSA TTCAATTTGTT AQGAALPRTFGQG CAAAGGACTC SVGDRVTISC TTCTACAAAGG TKVEIKR ATCAGCCGCTT RASQWIGSQL ACTCATCAGCC AAAEQKLISEEDL GGGATGAAAC SWYQQKPGE GCTTGGGATGA N* (SEQ ID NO: 396) TCTGTTAGATA APKLLIMWR AACTCTGTTAG AATTCTACACT SSLQSGVPSR ATAAATTCTAC GAACTATATCA FSGSGSGTDF ACTGAACTATA ACAACTGAAC TLTISSLQPED TCAACAACTGA GATCTAGAGGC FATYYCAQG ACGATCTAGA TTGCGTTATTC AALPRTFGQ GGCTTGCGTTA AGGGTGTAGG GTKVEIKR TTCAGGGTGTA AGTTACTGAAA (SEQ ID GGAGTTACTGA CTCCCCTAATG NO: 398) AACTCCCCTAA AAAGAAGATT TGAAAGAAGA CAATTCTAGCC TTCAATTCTAG GTTAGAAAATA CCGTTAGAAA CTTTCAGCGTA ATACTTTCAGC TCACATTGTAT GTATCACATTG TTAAAGGAAA TATTTAAAGGA AGAAATACTCC AAAGAAATAC CCATGTGCATG TCCCCATGTGC GGAGGTGGTTA ATGGGAGGTG GAGCAGAAAT GTTAGAGCAG TATGAGGTCCT AAATTATGAG TCTCTCTTTCT GTCCTTCTCTC ACGAATTTGCA TTTCTACGAAT AGAATCTTTGA TTGCAAGAATC GATCTAAGGA TTTGAGATCTA AACCGTCGCTG AGGAAACCGT CTCCATCTGAC CGCTGCTCCAT ATCCAGATGAC CTGACATCCAG CCAGTcTCCAT ATGACCCAGTc CCTCCCTGTCT TCCATCCTCCC GCATCTGTAGG TGTCTGCATCT AGACCGTGTCA GTAGGAGACC CCATCTCTTGC GTGTCACCATC CGGGCAAGTC TCTTGCCGGGC AGTGGATTGGG AAGTCAGTGG TCTCAGTTATC ATTGGGTCTCA TTGGTACCAGC GTTATCTTGGT AGAAACCAGG ACCAGCAGAA GGAAGCCCCTA ACCAGGGGAA AGCTCCTGATC GCCCCTAAGCT ATGTGGCGTTC CCTGATCATGT CTCGTTGCAAA GGCGTTCCTCG GTGGGGTCCCA TTGCAAAGTGG TCACGTTTCAG GGTCCCATCAC TGGCAGTGGAT GTTTCAGTGGC CTGGGACAGAT AGTGGATCTGG TTCACTCTCAC GACAGATTTCA CATCAGCAGTC CTCTCACCATC TGCAACCTGAA AGCAGTCTGCA GATTTTGCTAC ACCTGAAGATT GTACTACTGTG TTGCTACGTAC CTCAGGGTGCG TACTGTGCTCA GCGTTGCCTAG GGGTGCGGCG GACGTTCGGCC TTGCCTAGGAC AAGGGACCAA GTTCGGCCAAG GGTGGAAATC GGACCAAGGT AAACGGGCGG GGAAATCAAA CCGCAGAACA CGG (SEQ ID AAAACTCATC NO: 399) TCAGAAGAGG ATCTGAATTA A (SEQ ID NO: 397) DMS7325 CDLPQTHSLGSRRT TGCGACTTGCC CDLPQTHSLG TGCGACTTGCC (IFNα2b- LMLLAQMRRISLFS ACAGACACAT SRRTLMLLA ACAGACACAT DOM7h- CLKDRHDFGFPQE AGTTTGGGATC QMRRISLFSC AGTTTGGGATC 11) EFGNQFQKAETIPV AAGAAGAACA LKDRHDFGFP AAGAAGAACA LHEMIQQIFNLFST TTGATGTTATT QEEFGNQFQ TTGATGTTATT KDSSAAWDETLLD AGCACAAATG KAETIPVLHE AGCACAAATG KFYTELYQQLNDL CGTAGAATTTC MIQQIFNLFS CGTAGAATTTC EACVIQGVGVTETP TTTGTTCTCTT TKDSSAAWD TTTGTTCTCTT LMKEDSILAVRKY GTCTAAAGGAC ETLLDKFYTE GTCTAAAGGA FQRITLYLKEKKYS CGTCACGACTT LYQQLNDLE CCGTCACGACT PCAWEVVRAEIMR CGGATTCCCTC ACVIQGVGV TCGGATTCCCT SFSLSTNLQESLRS AGGAAGAGTTT TETPLMKEDS CAGGAAGAGT KETVAAPSDIQMT GGAAACCAATT ILAVRKYFQR TTGGAAACCA QSPSSLSASVGDRV CCAAAAAGCA ITLYLKEKKY ATTCCAAAAA TITCRASRPIGTTLS GAAACTATTCC SPCAWEVVR GCAGAAACTA WYQQKPGKAPKLL TGTCTTGCACG AEIMRSFSLS TTCCTGTCTTG IWFGSRLQSGVPSR AAATGATCCAG TNLQESLRSK CACGAAATGA FSGSGSGTDFTLTIS CAAATATTCAA ETVAAPSDIQ TCCAGCAAATA SLQPEDFATYYCA TTTGTTTTCTA MTQSPSSLSA TTCAATTTGTT QAGTHPTTFGQGT CAAAGGACTC SVGDRVTITC TTCTACAAAGG KVEIKR ATCAGCCGCTT RASRPIGTTL ACTCATCAGCC AAAEQKLISEEDL GGGATGAAAC SWYQQKPGK GCTTGGGATGA N* (SEQ ID NO: 400) TCTGTTAGATA APKLLIWFGS AACTCTGTTAG AATTCTACACT RLQSGVPSRF ATAAATTCTAC GAACTATATCA SGSGSGTDFT ACTGAACTATA ACAACTGAAC LTISSLQPEDF TCAACAACTGA GATCTAGAGGC ATYYCAQAG ACGATCTAGA TTGCGTTATTC THPTTFGQGT GGCTTGCGTTA AGGGTGTAGG KVEIKR (SEQ TTCAGGGTGTA AGTTACTGAAA ID NO: 402) GGAGTTACTGA CTCCCCTAATG AACTCCCCTAA AAAGAAGATT TGAAAGAAGA CAATTCTAGCC TTCAATTCTAG GTTAGAAAATA CCGTTAGAAA CTTTCAGCGTA ATACTTTCAGC TCACATTGTAT GTATCACATTG TTAAAGGAAA TATTTAAAGGA AGAAATACTCC AAAGAAATAC CCATGTGCATG TCCCCATGTGC GGAGGTGGTTA ATGGGAGGTG GAGCAGAAAT GTTAGAGCAG TATGAGGTCCT AAATTATGAG TCTCTCTTTCT GTCCTTCTCTC ACGAATTTGCA TTTCTACGAAT AGAATCTTTGA TTGCAAGAATC GATCTAAGGA TTTGAGATCTA AACCGTCGCTG AGGAAACCGT CTCCATCTGAC CGCTGCTCCAT ATCCAGATGAC CTGACATCCAG CCAGTCTCCAT ATGACCCAGTC CCTCCCTGTCT TCCATCCTCCC GCATCTGTAGG TGTCTGCATCT AGACCGTGTCA GTAGGAGACC CCATCACTTGC GTGTCACCATC CGGGCAAGTC ACTTGCCGGGC GTCCGATTGGG AAGTCGTCCGA ACGACGTTAAG TTGGGACGAC TTGGTACCAGC GTTAAGTTGGT AGAAACCAGG ACCAGCAGAA GAAAGCCCCTA ACCAGGGAAA AGCTCCTGATC GCCCCTAAGCT TGGTTTGGTTC CCTGATCTGGT CCGGTTGCAAA TTGGTTCCCGG GTGGGGTCCCA TTGCAAAGTGG TCACGTTTCAG GGTCCCATCAC TGGCAGTGGAT GTTTCAGTGGC CTGGGACAGAT AGTGGATCTGG TTCACTCTCAC GACAGATTTCA CATCAGCAGTC CTCTCACCATC TGCAACCTGAA AGCAGTCTGCA GATTTTGCTAC ACCTGAAGATT GTACTACTGTG TTGCTACGTAC CGCAGGCTGG TACTGTGCGCA GACGCATCCTA GGCTGGGACG CGACGTTCGGC CATCCTACGAC CAAGGGACCA GTTCGGCCAAG AGGTGGAAAT GGACCAAGGT CAAACGGGCG GGAAATCAAA GCCGCAGAAC CGG (SEQ ID AAAAACTCAT NO: 403) CTCAGAAGAG GATCTGAATT AA (SEQ ID NO: 401) DMS7326 CDLPQTHSLGSRRT TGCGACTTGCC CDLPQTHSLG TGCGACTTGCC (IFNα2b- LMLLAQMRRISLFS ACAGACACAT SRRTLMLLA ACAGACACAT DOM7h- CLKDRHDFGFPQE AGTTTGGGATC QMRRISLFSC AGTTTGGGATC 11-12) EFGNQFQKAETIPV AAGAAGAACA LKDRHDFGFP AAGAAGAACA LHEMIQQIFNLF STTTGATGTTATT QEEFGNQFQ TTGATGTTATT KDSSAAWDETLLD AGCACAAATG KAETIPVLHE AGCACAAATG KFYTELYQQLNDL CGTAGAATTTC MIQQIFNLFS CGTAGAATTTC EACVIQGVGVTETP TTTGTTCTCTT TKDSSAAWD TTTGTTCTCTT LMKEDSILAVRKY GTCTAAAGGAC ETLLDKFYTE GTCTAAAGGA FQRITLYLKEKKYS CGTCACGACTT LYQQLNDLE CCGTCACGACT PCAWEVVRAEIMR CGGATTCCCTC ACVIQGVGV TCGGATTCCCT SFSLSTNLQESLRS AGGAAGAGTTT TETPLMKEDS CAGGAAGAGT KETVAAPSDIQMT GGAAACCAATT ILAVRKYFQR TTGGAAACCA QSPSSLSASVGDRV CCAAAAAGCA ITLYLKEKKY ATTCCAAAAA TITCRASRPIGTML GAAACTATTCC SPCAWEVVR GCAGAAACTA SWYQQKPGKAPKL TGTCTTGCACG AEIMRSFSLS TTCCTGTCTTG LILFGSRLQSGVPS AAATGATCCAG TNLQESLRSK CACGAAATGA RFSGSGSGTDFTLT CAAATATTCAA ETVAAPSDIQ TCCAGCAAATA ISSLQPEDFATYYC TTTGTTTTCTA MTQSPSSLSA TTCAATTTGTT AQAGTHPTTFGQG CAAAGGACTC SVGDRVTITC TTCTACAAAGG TKVEIKR ATCAGCCGCTT RASRPIGTML ACTCATCAGCC AAAEQKLISEEDL GGGATGAAAC SWYQQKPGK GCTTGGGATGA N* (SEQ ID NO: 404) TCTGTTAGATA APKLLILFGS AACTCTGTTAG AATTCTACACT RLQSGVPSRF ATAAATTCTAC GAACTATATCA SGSGSGTDFT ACTGAACTATA ACAACTGAAC LTISSLQPEDF TCAACAACTGA GATCTAGAGGC ATYYCAQAG ACGATCTAGA TTGCGTTATTC THPTTFGQGT GGCTTGCGTTA AGGGTGTAGG KVEIKR (SEQ TTCAGGGTGTA AGTTACTGAAA ID NO: 406) GGAGTTACTGA CTCCCCTAATG AACTCCCCTAA AAAGAAGATT TGAAAGAAGA CAATTCTAGCC TTCAATTCTAG GTTAGAAAATA CCGTTAGAAA CTTTCAGCGTA ATACTTTCAGC TCACATTGTAT GTATCACATTG TTAAAGGAAA TATTTAAAGGA AGAAATACTCC AAAGAAATAC CCATGTGCATG TCCCCATGTGC GGAGGTGGTTA ATGGGAGGTG GAGCAGAAAT GTTAGAGCAG TATGAGGTCCT AAATTATGAG TCTCTCTTTCT GTCCTTCTCTC ACGAATTTGCA TTTCTACGAAT AGAATCTTTGA TTGCAAGAATC GATCTAAGGA TTTGAGATCTA AACCGTCGCTG AGGAAACCGT CTCCATCTGAC CGCTGCTCCAT ATCCAGATGAC CTGACATCCAG CCAGTCTCCAT ATGACCCAGTC CCTCCCTGTCT TCCATCCTCCC GCATCTGTAGG TGTCTGCATCT AGACCGTGTCA GTAGGAGACC CCATCACTTGC GTGTCACCATC CGGGCAAGTC ACTTGCCGGGC GTCCGATTGGG AAGTCGTCCGA ACGATGTTAAG TTGGGACGATG TTGGTACCAGC TTAAGTTGGTA AGAAACCAGG CCAGCAGAAA GAAAGCCCCTA CCAGGGAAAG AGCTCCTGATC CCCCTAAGCTC TTGTTTGGTTC CTGATCTTGTT CCGGTTGCAAA TGGTTCCCGGT GTGGGGTCCCA TGCAAAGTGG TCACGTTTCAG GGTCCCATCAC TGGCAGTGGAT GTTTCAGTGGC CTGGGACAGAT AGTGGATCTGG TTCACTCTCAC GACAGATTTCA CATCAGCAGTC CTCTCACCATC TGCAACCTGAA AGCAGTCTGCA GATTTTGCTAC ACCTGAAGATT GTACTACTGTG TTGCTACGTAC CGCAGGCTGG TACTGTGCGCA GACGCATCCTA GGCTGGGACG CGACGTTCGGC CATCCTACGAC CAAGGGACCA GTTCGGCCAAG AGGTGGAAAT GGACCAAGGT CAAACGGGCG GGAAATCAAA GCCGCAGAAC CGG (SEQ ID AAAAACTCAT NO: 407) CTCAGAAGAG GATCTGAATT AA (SEQ ID NO: 405 DMS7327 CDLPQTHSLGSRRT TGCGACTTGCC CDLPQTHSLG TGCGACTTGCC (IFNα2b- LMLLAQMRRISLFS ACAGACACAT SRRTLMLLA ACAGACACAT DOM7h- CLKDRHDFGFPQE AGTTTGGGATC QMRRISLFSC AGTTTGGGATC 11-15) EFGNQFQKAETIPV AAGAAGAACA LKDRHDFGFP AAGAAGAACA LHEMIQQIFNLF STTTGATGTTATT QEEFGNQFQ TTGATGTTATT KDSSAAWDETLLD AGCACAAATG KAETIPVLHE AGCACAAATG KFYTELYQQLNDL CGTAGAATTTC MIQQIFNLFS CGTAGAATTTC EACVIQGVGVTETP TTTGTTCTCTT TKDSSAAWD TTTGTTCTCTT LMKEDSILAVRKY GTCTAAAGGAC ETLLDKFYTE GTCTAAAGGA FQRITLYLKEKKYS CGTCACGACTT LYQQLNDLE CCGTCACGACT PCAWEVVRAEIMR CGGATTCCCTC ACVIQGVGV TCGGATTCCCT SFSLSTNLQESLRS AGGAAGAGTTT TETPLMKEDS CAGGAAGAGT KETVAAPSDIQMT GGAAACCAATT ILAVRKYFQR TTGGAAACCA QSPSSLSASVGDRV CCAAAAAGCA ITLYLKEKKY ATTCCAAAAA TITCRASRPIGTML GAAACTATTCC SPCAWEVVR GCAGAAACTA SWYQQKPGKAPKL TGTCTTGCACG AEIMRSFSLS TTCCTGTCTTG LILAFSRLQSGVPS AAATGATCCAG TNLQESLRSK CACGAAATGA RFSGSGSGTDFTLT CAAATATTCAA ETVAAPSDIQ TCCAGCAAATA ISSLQPEDFATYYC TTTGTTTTCTA MTQSPSSLSA TTCAATTTGTT AQAGTHPTTFGQG CAAAGGACTC SVGDRVTITC TTCTACAAAGG TKVEIKR ATCAGCCGCTT RASRPIGTML ACTCATCAGCC AAAEQKLISEEDL GGGATGAAAC SWYQQKPGK GCTTGGGATGA N* (SEQ ID NO: 408) TCTGTTAGATA APKLLILAFS AACTCTGTTAG AATTCTACACT RLQSGVPSRF ATAAATTCTAC GAACTATATCA SGSGSGTDFT ACTGAACTATA ACAACTGAAC LTISSLQPEDF TCAACAACTGA GATCTAGAGGC ATYYCAQAG ACGATCTAGA TTGCGTTATTC THPTTFGQGT GGCTTGCGTTA AGGGTGTAGG KVEIKR (SEQ TTCAGGGTGTA AGTTACTGAAA ID NO: 410) GGAGTTACTGA CTCCCCTAATG AACTCCCCTAA AAAGAAGATT TGAAAGAAGA CAATTCTAGCC TTCAATTCTAG GTTAGAAAATA CCGTTAGAAA CTTTCAGCGTA ATACTTTCAGC TCACATTGTAT GTATCACATTG TTAAAGGAAA TATTTAAAGGA AGAAATACTCC AAAGAAATAC CCATGTGCATG TCCCCATGTGC GGAGGTGGTTA ATGGGAGGTG GAGCAGAAAT GTTAGAGCAG TATGAGGTCCT AAATTATGAG TCTCTCTTTCT GTCCTTCTCTC ACGAATTTGCA TTTCTACGAAT AGAATCTTTGA TTGCAAGAATC GATCTAAGGA TTTGAGATCTA AACCGTCGCTG AGGAAACCGT CTCCATCTGAC CGCTGCTCCAT ATCCAGATGAC CTGACATCCAG CCAGTCTCCAT ATGACCCAGTC CCTCCCTGTCT TCCATCCTCCC GCATCTGTAGG TGTCTGCATCT AGACCGTGTCA GTAGGAGACC CCATCACTTGC GTGTCACCATC CGGGCAAGTC ACTTGCCGGGC GTCCGATTGGG AAGTCGTCCGA ACGATGTTAAG TTGGGACGATG TTGGTACCAGC TTAAGTTGGTA AGAAACCAGG CCAGCAGAAA GAAAGCCCCTA CCAGGGAAAG AGCTCCTGATC CCCCTAAGCTC CTTGCTTTTTC CTGATCCTTGC CCGTTTGCAAA TTTTTCCCGTT GTGGGGTCCCA TGCAAAGTGG TCACGTTTCAG GGTCCCATCAC TGGCAGTGGAT GTTTCAGTGGC CTGGGACAGAT AGTGGATCTGG TTCACTCTCAC GACAGATTTCA CATCAGCAGTC CTCTCACCATC TGCAACCTGAA AGCAGTCTGCA GATTTTGCTAC ACCTGAAGATT GTACTACTGCG TTGCTACGTAC CGCAGGCTGG TACTGCGCGCA GACGCATCCTA GGCTGGGACG CGACGTTCGGC CATCCTACGAC CAAGGGACCA GTTCGGCCAAG AGGTGGAAAT GGACCAAGGT CAAACGGGCG GGAAATCAAA GCCGCAGAAC CGG (SEQ ID AAAAACTCAT NO: 411) CTCAGAAGAG GATCTGAATT AA (SEQ ID NO: 409) The amino acid and nucleotide sequences highlighted in bold represents the cloning site and MYC tag. * represents the stop codon at the end of the gene.

Affinity Determination and Biophysical Characterisation:

To determine the binding affinity (K_(D)) of the ALBUDAB™-IFNα2b fusion proteins to each serum albumin; purified fusion proteins were analysed by BiaCore™ over albumin (immobilised by primary-amine coupling onto CM5 chips; BiaCore™) using fusion protein concentrations from 5000 nM to 39 nM (5000 nM, 2500 nM, 1250 nM, 625 nM, 312 nM, 156 nM, 78 nM, 39 nM) in HBS-EP BiaCore™ buffer.

TABLE 12 Affinity to SA Affinity to ALBUDAB ™ Fusion SA (nM) Kd Ka Rat DOM7h-14 IFNα2b 350 4.500E−02  1.28E+05 DOM7h-14-10 IFNα2b 16 4.970E−03  5.90E+05 DOM 7h-14-18 IFNα2b 780 2.127E−01  5.80E+05 DOM 7h-14-19 IFNα2b 1900 1.206E−01  7.96E+04 DOM 7h-11 IFNα2b 6000 7.500E−01  nd DOM 7h-11-12 IFNα2b 1700 3.100E−01  1.30E+05 DOM 7h-11-15 IFNα2b 200 1.660E−02  1.50E+05 Cyno DOM 7h-14 IFNα2b 60 1.32E−02  5.0E+05 DOM 7h-14-10 IFNα2b 19 7.05E−03 4.50E+05 DOM 7h-14-18 IFNα2b no binding no binding no binding DOM 7h-14-19 IFNα2b 520 8.47E−02 2.73E+05 DOM 7h-11 IFNα2b 3300 3.59E−01 1.20E+05 DOM 7h-11-12 IFNα2b 630 3.45E−01 7.00E+05 DOM 7h-11-15 IFNα2b 15 4.86E−03 3.60E+05 Mouse DOM 7h-14 IFNα2b 240 3.21E−02 1.50E+06 DOM 7h-14-10 IFNα2b 60 3.45E−02 6.86E+05 DOM 7h-14-18 IFNα2b 180 1.50E−01 9.84E+05 DOM 7h-14-19 IFNα2b 490 4.03E−02 1.19E+05 DOM 7h-11 IFNα2b 6000 1.55E−01 nd DOM 7h-11-12 IFNα2b 150 9.49E−02 6.30E+05 DOM 7h-11-15 IFNα2b 28 6.69E−03 2.80E+05 Human DOM 7h-14 IFNα2b 244 2.21E−02 9.89E+04 DOM 7h-14-10 IFNα2b 32 6.58E−03 3.48E+05 DOM 7h-14-18 IFNα2b 470 2.75E−01 6.15E+05 DOM 7h-14-19 IFNα2b 350 4.19E−02 1.55E+05 DOM 7h-11 IFNα2b 670 2.02E−01 7.00E+05 DOM 7h-11-12 IFNα2b 500 1.66E−01 3.90E+05 DOM 7h-11-15 IFNα2b 10 1.87E−03 3.50E+05 When IFNα2b is linked to the ALBUDAB ™ variants, in all cases the affinity of ALBUDAB ™ binding to serum albumin is reduced. DOM7h-14-10 and DOM7-11-15 retain improved binding affinity to serum albumin across species compared to parent. DOM7h-11-12 also shows improved binding affinity to serum albumin across species compared to parent.

TABLE 13 Biophysical Characterisation Biophysical Characterisation was carried out by SEC MALLS and DSC as described above for the single ALBUDABs ™ Biophysical parameters DMS SEC DSC ALBUDAB ™ Fusion number MALLS Tm(° C.) DOM 7h-14 IFNα2b DMS7321 M/D 58-65 DOM 7h-14-10 IFNα2b DMS7322 M/D 55-65 DOM 7h-14-18 IFNα2b DMS7323 M/D 55-65 DOM 7h-14-19 IFNα2b DMS7324 M/D 59-66 DOM 7h-11 IFNα2b DMS7325 M/D 65.8-66.2 DOM 7h-11-12 IFNα2b DMS7326 M/D  67-67.3 DOM 7h-11-15 IFNα2b DMS7327 M/D 56.3-66.2 M/D indicates a monomer/dimer equilibrium as detected by SEC MALLS We observed expression for all clones in Tabale 13 in the range of 17.5 to 54 mg/L in HEK293. For IFNα2b-DOM7h-14 and IFNα2b-DOM7h-11 variants, favorable biophysical parameters and expression levels were maintained during affinity maturation.

PK Determination for ALBUDAB™-IFNα2b Fusions

ALBUDABs™ IFNα2b fusions DMS7321 (IFNα2b-DOM7h-14) DMS7322 (IFNα2b-DOM7h-14-10) DMS7323 (IFNα2b-DOM7h-14-18), DMS7324 (IFNα2b-DOM7h-14-19), DMS7325 (IFNα2b-DOM7h-11), DMS7326 (IFNα2b-DOM7h-11-12), DMS7327 (IFNα2b-DOM7h-11-15) were expressed with the myc tag at 20-50 mg quantities in HEK293 cells and purified from culture supernatant using protein L affinity resin and eluted with 100 mM glycine pH2. The proteins were concentrated to greater than 1 mg/ml, buffer exchanged into Dulbecco's PBS and endotoxin depleted using Q spin columns (Vivascience).

For Rat PK, IFN-ALBUDABs™ were dosed as single i.v injections at 2.0 mg/kg using 3 rats per compound. Serum samples were taken at 0.16, 1, 4, 8, 24, 48, 72, 120, 168 hrs. Analysis of serum levels was by EASY ELISA according to manufacturers instructions (GE Healthcare, catalogue number RPN5960).

For Mouse PK, DMS7322 (IFN2b-DOM7h-14-10) DMS7325 (IFN2b-DOM7h-11), DMS7326 (IFN2b-DOM7h-11-12), DMS7327 (IFN2b-DOM7h-11-15) all with myc tags were dosed as single i.v injections at 2.0 mg/kg per dose group of 3 subjects and serum samples taken at 10 mins; 1 h; 8h; 24h; 48h; 72h; 96h. Analysis of serum levels was by EASY ELISA according to manufacturers instructions (GE Healthcare, catalogue number RPN5960).

TABLE 14 PK parameters Albumin AUC CL t½ Vz Species ALBUDAB ™ Fusion K_(D) (nM) h × ug/ml ml/h/kg h ml/kg Rat 7h-14 IFNα2b 350 832.1 2.4 27 94.5 7h-14-10 IFNα2b 16 1380.7 1.5 35.8 75.2 7h-14-18 IFNα2b 780 691.2 2.9 22.4 93.7 7h-14-19 IFNα2b 1900 969.4 2.2 25 78.7 7h-11 IFNα2b 6000 327.9 6.5 11 101.9 7h-11-12 IFNα2b 1700 747.1 2.8 25.8 104.7 7h-11-15 IFNα2b 200 1118.7 1.8 39.5 103.6 mouse 7h-14 IFNα2b 240 761.2 2.6 30.4 115.3 7h-14-10 IFNα2b 60 750.5 2.7 30.9 118.6 7h-11 IFNα2b 6000 493.9 4.0 8.8 51.2 7h-11-12 IFNα2b 150 439.6 4.5 21.5 140.9 7h-11-15 IFNα2b 28 971.8 2.1 33.6 99.6 Pharmacokinetic parameters derived from rat and mouse studies were fitted using a non-compartmental model. Key: AUC: Area under the curve from dosing time extrapolated to infinity; CL: clearance; t½: is the time during which the blood concentration is halved; Vz: volume of distribution based on the terminal phase. IFNα2b -ALBUDABs ™ were tested in rat and mouse. For all IFNα2b-DOM7h-11 variant fusion proteins in both rat and mouse, t½ is improved compared to parent. The improvement in t½ correlates with the improved in vitro K_(D) to serum albumin. For IFNα2b-DOM7h-14-10 variants, the improvement in in vitro K_(D) to serum albumin also correlated to an improvement in t½ in rat. All IFNα2b -ALBUDAB ™ fusion proteins exhibit a 5 to 10-fold decrease in the binding to RSA compared to the single ALBUDAB ™. This effect is more pronounced (i.e. 10-fold) for the DOM7h-14 series than the DOM7h-11 series (only 5-fold decrease).

Example 8: Further ALBUDAB™ Fusions with Proteins, Peptides and NCEs

Various ALBUDABs™ fused to other chemical entities namely domain antibodies (dAbs), peptides and NCEs were tested. The results are shown in table 15.

TABLE 15 PK parameters Albumin AUC CL t½ Vz Species ALBUDAB ™ Fusion K_(D) (nM) h × ug/ml ml/h/kg h ml/kg Rat DOM7h-14 Exendin-4 2400 18 57.1 11 901.9 DOM7h-14-10 Exendin-4 19 43.6 23.1 22.1 740.3 DOM7h-14-18 Exendin-4 16000 16.9 75.7 9.4 1002.5 DOM7h-14-19 Exendin-4 17000 31.4 32.5 11.9 556.7 DOM7h-11 Exendin-4 24000 6.1 168 7.1 1684.1 DOM7h-11-12 Exendin-4 1400 24.2 59.9 13 1068.7 DOM7h-11-15 Exendin-4 130 36.3 27.6 19.3 765.7 DOM7h14-10 NCE-GGGGSC 62 DOM7h14-10 NCE-TVAAPSC 35 Human DOM7h-14 NCE 204 mouse DOM7h-11 DOM1m-21-23 234 10.7 4.7 72.5 DOM7h-11-12 DOM1m-21-23 755 3.3 18 86.2 DOM7h-11-15 DOM1m-21-23 1008 2.5 17.4 62.4 Key: DOM1m-21-23 is an anti-TNFR1 dAb, Exendin-4 is a peptide (a GLP-1 agonist) of 39 amino acids length. NCE, NCE-GGGGSC and NCE-TVAAPSC are described below. Previously we have described the use of genetic fusions with an albumin-binding dAb (ALBUDAB ™) to extend the PK half-life of anti-TNFR1 dAbs in vivo (see, eg, WO04003019, WO2006038027, WO2008149148). Reference is made to the protocols in these PCT applications. In the table above, DOM1m-21-23 is an anti-mouse TNFR1 dAb.

To produce genetic fusions of exendin-4 or with DOM7h-14 (or other ALBUDAB′) which binds serum albumin, the exendin-4-linker-ALBUDAB′ sequence was cloned into the pTT-5 vector (obtainable from CNRC, Canada). In each case the exendin-4 was at the 5′ end of the construct and the dAb at the 3′ end. The linker was a (G4S)3 linker. Endotoxin-free DNA was prepared in E. coli using alkaline lysis (using the endotoxin-free plasmid Giga kit, obtainable from Qiagen CA) and used to transfect HEK293E cells (obtainable from CNRC, Canada). Transfection was into 250 ml/flask of HEK293E cells at 1.75×10⁶ cells/ml using 333 ul of 293 fectin (Invotrogen) and 250 ug of DNA per flask and expression was at 30° C. for 5 days. The supernatant was harvested by centrifugation and purification was by affinity purification on protein L. Protein was batch bound to the resin, packed on a column and washed with 10 column volumes of PBS. Protein was eluted with 50 ml of 0.1M glycine pH2 and neatralised with Tris pH8. Protein of the expected size was identified on an SDS-PAGE gel.

NCE ALBUDAB™ Fusions:

A new chemical entity (NCE) ALBUDAB™ fusion was tested. The NCE, a small molecule ADAMTS-4 inhibitor was synthesised with a PEG linker (PEG 4 linker (ie 4 PEG molecules before the maleimide) and a maleimide group for conjugation to the ALBUDAB™. Conjugation of the NCE to the ALBUDAB™ is via an engineered cystine residue at amino acid position R108C, or following a 5 amino acid (GGGGSC) or 6 amino acid (TVAAPSC (SEQ ID NO: 419)) spacer engineered at the end of the ALBUDAB™. Briefly, the AALBUDAB™ was reduced with TCEP (Pierce, Catalogue Number 77720), desalted using a PD10 column (GE healthcare) into 25 mM Bis-Tris, 5 mM EDTA, 10% (v/v) glycerol pH6.5. A 5 fold molar excess of maleimide activated NCE was added in DMSO not to exceed 10% (V/V) final concentration. The reaction was incubated over night at room temperature and dialysed extensively into 20 mM Tris pH7.4

PEG Linker:

Sequences:

DOM7h-14 R108C: (SEQ ID NO: 412) DIQMTQSPSSLSASVGDRVTITCRASQWIGSQLSWYQQKPGKAPKLLIMW RSSLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQGLRHPKTFGQ GTKVEIKC Nucleotide: (SEQ ID NO: 413) GACATCCAGATGACCCAGTCTCCATCCTCCCTGTCTGCATCTGTAGGAGA CCGTGTCACCATCACTTGCCGGGCAAGTCAGTGGATTGGGTCTCAGTTAT CTTGGTACCAGCAGAAACCAGGGAAAGCCCCTAAGCTCCTGATCATGTGG CGTTCCTCGTTGCAAAGTGGGGTCCCATCACGTTTCAGTGGCAGTGGATC TGGGACAGATTTCACTCTCACCATCAGCAGTCTGCAACCTGAAGATTTTG CTACGTACTACTGTGCTCAGGGTTTGAGGCATCCTAAGACGTTCGGCCAA GGGACCAAGGTGGAAATCAAATGC

See table 5 for the sequences of DOM7h-14-10/TVAAPSC and DOM7h-14-10/GGGGSC (ie, DOM7h-14-10/G4 SC).

NCE-ALBUDABs™ DOM7h-14-10 GGGGSC(SEQ ID NO: 62) and DOM7h14-10 TVAAPSC, exhibit a 5 to 10 fold decrease in in vitro affinity (K_(D)) to RSA as determined by BiaCore™ when fused to the chemical entity. PK data are not available for these molecules yet.

dAb-ALBUDAB™ fusion: the 2 DOM7h-11 ALBUDABs™ with the highest affinity to RSA experience a 2-fold decrease in affinity to RSA as on BiaCore™ when fused to a therapeutic domain antibody (DOM1m-21-23) compared to the unfused ALBUDAB™. The DOM7h-11 clone shows a micromolar K_(D) when fused (2.8 uM) as well as when unfused (˜5 uM).

Exendin 4-ALBUDAB™ fusion: the effect of fusing the ALBUDABs™ to a peptide on the binding ability to RSA is about 10-fold, apart from DOM7h-14-10, which only shows a 4-fold decrease in binding. The effect, however, is more pronounced for the DOM7h-14 series (except DOM7h-14-10) than it appears to be for the DOM7h-11 series.

For all the above data, the T1/2 of the fusion increased with improved affinity to the species' SA.

We generally classify ALBUDAB™-therapeutics as being therapeutically amenable (for treatment and/or prophylaxis of diseases, conditions or indications) when the ALBUDAB™-drug fusions show an affinity range (K_(D)) of from 0.1 nM to 10 mM for serum albumin binding.

We define the therapeutic ranges of ALBUDABs™ and ALBUDAB™ fusions (Protein-ALBUDABs™ for example IFNα2b-DOM7h-14-10; Peptide-ALBUDABs™ for example Exendin-4-DOM7h-14-10; dAb-ALBUDABs™ for example DOM1m21-23-DOM7h11-15; NCE-ALBUDAB™ for example ADAMTS-4-DOM7h-14-10) as follows: Affinity (K_(D)) ranges that are useful for therapy of chronic or acute conditions, diseases or indictions are shown. Also shown are affinity ranges marked as “intermediate”. ALBUDABs™ and fusions in this range have utility for chronic or acute diseases, conditions or indications. In this way, the affinity of the ALBUDAB™ or fusion for serum albumin can be tailored or chosen according to the disease, condition or indication to be addressed. As described above, the invention provides ALBUDABs™ with affinities that allow for each ALBUDAB™ to be categorised as “high affinity”, “medium affinity” or “low affinity”, thus enabling the skilled person to select the appropriate ALBUDAB™ of the invention according to the therapy at hand. See FIG. 2.

Example 9: DOM7h-11-15^(S12P) Sequences Amino Acid Sequence of DOM7h-11-15^(S12P)

(SEQ ID NO: 414) DIQMTQSPSSLPASVGDRVTITCRASRPIGTMLSWYQQKPGKAPKLLILA FSRLQSGVPSRFSGSGSGTDFTLTISSLQPEDFATYYCAQAGTHPTTFGQ GTKVEIKR

An aspect of the invention provides a nucleic acid comprising the nucleotide sequence of DOM7h-11-15^(S12P) or a nucleotide sequence that is at least 80% identical to said selected sequence. DOM7h-11-15^(S12P) was produced using the following nucleic acid sequence (the underlined C denotes the change (versus the nucleic acid encoding DOM7h-11-15) leading to a proline at position 12):—

(SEQ ID NO: 415) GACATCCAGATGACCCAGTCTCCATCCTCCCTGCCTGCATCTGTAGGAGA CCGTGTCACCATCACTTGCCGGGCAAGTCGTCCGATTGGGACGATGTTAA GTTGGTACCAGCAGAAACCAGGGAAAGCCCCTAAGCTCCTGATCCTTGCT TTTTCCCGTTTGCAAAGTGGGGTCCCATCACGTTTCAGTGGCAGTGGATC TGGGACAGATTTCACTCTCACCATCAGCAGTCTGCAACCTGAAGATTTTG CTACGTACTACTGCGCGCAGGCTGGGACGCATCCTACGACGTTCGGCCAA GGGACCAAGGTGGAAATCAAACGG

DOM7h-11-15^(S12P) was constructed by using DOM7h-11-15 as a template in a PCR where a primer was used to introduce the S12P mutation. The primer sequence is:—

(SEQ ID NO: 416) GCAACAGCGTCGACGGACATCCAGATGACCCAGTCTCCATCCTCCCTGCC TGCATCTGTAGG

An alternative aspect of the invention provides a nucleic acid comprising the nucleotide sequence of SEQ ID NO: 415 or a nucleotide sequence that is at least 80% identical to said selected sequence. In one embodiment, DOM7h-11-15^(S12P) is encoded by, and expressed from, a vector that contains a linker region and a C-terminal sequence encoding a protein or peptide drug or a single variable domain or other antibody fragment to make the in-line protein fusion product. The linker, in one embodiment, comprises the amino acid sequence TVA, eg, TVAAPS (SEQ ID NO: 422). Other aspects of the invention are a vector comprising the nucleic acid; and an isolated host cell comprising the vector. The invention also provides a method of treating or preventing a disease or disorder in a patient, comprising administering at least one dose of DOM7h-11-15^(S12P) to said patient. 

1. An anti-serum albumin (SA) immunoglobulin single variable domain variant of DOM7h-11 (DOM7h-11 as shown in FIG. 1), wherein the variant comprises at least one mutation in the FW2/CDR2 junction (positions 49 to 51, numbering according to Kabat) compared to DOM7h-11, and wherein the variant has from 2 to 8 changes compared to the amino acid sequence of DOM7h-11.
 2. The variant of claim 1, wherein position 49 (according to Kabat) is Leu.
 3. The variant of claim 1, wherein position 50 (according to Kabat) is Ala or Trp.
 4. The variant of claim 1, wherein position 51 (according to Kabat) is Phe or Asn.
 5. The variant of claim 1, wherein the variant comprises an amino acid sequence that is identical to the amino acid sequence of a single variable domain selected from DOM7h-11-3 (SEQ ID NO: 5), DOM7h-11-15 (SEQ ID NO: 2), DOM7h-11-12 (SEQ ID NO: 1) and DOM7h-11-19 (SEQ ID NO: 4) or has up to 4 changes compared to the selected amino acid sequence, provided that the amino acid sequence of the variant has at least one mutation in the FW2/CDR2 junction.
 6. The variant of claim 1, wherein the variant comprises an amino acid sequence that is identical to the amino acid sequence of DOM7h-11-15^(S12P) (SEQ ID NO: 414) or has up to 4 changes compared to the amino acid sequence of DOM7h-11-15^(S12P), provided that the amino acid sequence of the variant has at least one mutation in the FW2/CDR2 junction.
 7. An anti-serum albumin (SA) immunoglobulin single variable domain variant of DOM7h-11, wherein the variant comprises a Met at position 32 (numbering according to Kabat) compared to DOM7h-11 (as shown in FIG. 1), and wherein the variant has from 0 to 4 further changes compared to the amino acid sequence of DOM7h-11.
 8. The variant of claim 7, wherein the variant comprises at least one mutation in the FW2/CDR2 junction (positions 49 to 51, numbering according to Kabat) compared to DOM7h-11 (as shown in FIG. 1).
 9. The variant of claim 7, wherein the variant comprises at least one mutation compared to DOM7h-11 (as shown in FIG. 1) selected from the following Position 49=L, Position 50=A or W, Position 51=F or N, Position 87=H, and Position 91=T.
 10. The variant of claim 7, wherein the variant comprises an amino acid sequence that is identical to the amino acid sequence of a single variable domain selected from DOM7h-11-12 (SEQ ID NO: 1), DOM7h-11-15 (SEQ ID NO: 2), DOM7h-11-18 (SEQ ID NO: 3) and DOM7h-11-19 (SEQ ID NO: 4) or has up to 4 changes compared to the selected amino acid sequence, provided that the amino acid sequence of the variant has Met at position
 32. 11. The variant of claim 7, wherein the variant comprises an amino acid sequence that is identical to the amino acid sequence of DOM7h-11-15^(S12P) (SEQ ID NO: 414) or has up to 4 changes compared to the selected amino acid sequence, provided that the amino acid sequence of the variant has Met at position
 32. 12. The variant of claim 1, wherein the variant comprises a binding site that specifically binds human SA with a dissociation constant (KD) of from about 0.1 to about 10000 nM, optionally from about 1 to about 6000 nM, as determined by surface plasmon resonance.
 13. The variant of claim 1, wherein the variant comprises a binding site that specifically binds human SA with an off-rate constant (K_(d)) of from about 1.5×10⁻⁴ to about 0.1 sec⁻¹, optionally from about 3×10⁻⁴ to about 0.1 sec⁻¹ as determined by surface plasmon resonance.
 14. The variant of claim 1, wherein the variant comprises a binding site that specifically binds human SA with an on-rate constant (K_(a)) of from about 2×10⁶ to about 1×10⁴M⁻¹ sec⁻¹, optionally from about 1×10⁶ to about 2×10⁴M⁻¹ sec⁻¹ as determined by surface plasmon resonance.
 15. The variant of claim 1, wherein the variant comprises a binding site that specifically binds Cynomolgus monkey SA with a dissociation constant (KD) of from about 0.1 to about 10000 nM, optionally from about 1 to about 6000 nM, as determined by surface plasmon resonance.
 16. The variant of claim 1, wherein the variant comprises a binding site that specifically binds Cynomolgus monkey SA with an off-rate constant (K_(d)) of from about 1.5×10⁻⁴ to about 0.1 sec⁻¹, optionally from about 3×10⁻⁴ to about 0.1 sec⁻¹ as determined by surface plasmon resonance.
 17. The variant of claim 1, wherein the variant comprises a binding site that specifically binds Cynomolgus monkey SA with an on-rate constant (K_(a)) of from about 2×10⁶ to about 1×10⁴M⁻¹ sec⁻¹, optionally from about 1×10⁶ to about 5×10³M⁻¹ sec⁻¹ as determined by surface plasmon resonance.
 18. A multispecific ligand comprising an anti-SA variant of claim 1 and a binding moiety that specifically binds a target antigen other than SA.
 19. An anti-SA variant single variable domain of claim 1, wherein the variable domain is conjugated to a drug (optionally an NCE drug), optionally wherein the selected variant is DOM7h-11-15 (SEQ ID NO: 2), DOM7h-11-15^(S12P) (SEQ ID NO: 414) or DOM7h-11-12 (SEQ ID NO: 1).
 20. A fusion protein comprising a polypeptide or peptide drug fused to a variant according to claim 1, optionally wherein the selected variant is DOM7h-11-15 (SEQ ID NO: 2), DOM7h-11-15^(S12P) (SEQ ID NO: 414) or DOM7h-11-12 (SEQ ID NO: 1).
 21. A fusion protein according to claim 20, wherein the fusion protein comprises a linker (eg, a linker comprising the amino acid sequence TVA, optionally TVAAPS) between the variant and the drug.
 22. A composition comprising a variant, fusion protein or ligand of claim 1 and a pharmaceutically acceptable diluent, carrier, excipient or vehicle.
 23. A nucleic acid comprising a nucleotide sequence encoding a variant according to claim
 1. 24. A nucleic acid comprising the nucleotide sequence of a DOM7h-11 variant selected from the nucleotide sequence of DOM7h-11-3 (SEQ ID NO: 5), DOM7h-11-15 (SEQ ID NO: 2), DOM7h-11-12 (SEQ ID NO: 1), DOM7h-11-18 (SEQ ID NO: 3) and DOM7h-11-19 (SEQ ID NO: 4) or a nucleotide sequence that is at least 80% identical to said selected sequence.
 25. A nucleic acid comprising the nucleotide sequence of DOM7h-11-15^(S12P) (SEQ ID NO: 414) or a nucleotide sequence that is at least 80% identical to said selected sequence.
 26. A vector comprising the nucleic acid of claim
 23. 27. An isolated host cell comprising the vector of claim
 26. 28. A method of treating or preventing a disease or disorder in a patient, comprising administering at least one dose of a variant according to claim 1 to said patient. 